Abstract

Yellow fever was transported during the slave trade in the 15th and 16th centuries from Africa to the Americas where the virus encountered favorable ecological conditions that allowed creation of a sustainable sylvatic cycle. Despite effective vector control and immunization programs for nearly a century, yellow fever epidemics reemerged in many Latin American countries, particularly Brazil. The emergence or reemergence of vector-borne diseases encompasses many intricate factors. Yellow fever outbreaks occur if at least three conditions are fulfilled: the introduction of the virus into a non-immune human community, presence of competent and anthropophilic vectors and insufficiency of prevention and/or adequate management of the growing outbreak. On the other hand, two weapons are available to constrain yellow fever: vector control and immunization. In contrast, yellow fever is absent from Asia and the Pacific despite the presence of the vector and the susceptibility of human populations to the virus. Based on a review of the global history of yellow fever and its epidemiology, the authors deliver some recommendations for improving the prevention of epidemics.

Keywords:
Yellow fever; Aedes aegypti; Haemagogus sp.; Sabethes sp. Vector; Arbovirus; Epidemiology; Brazil; Latin America; Africa

Background

Brazil has experienced an exceptional yellow fever (YF) outbreak since December 2016 ( Table 1 ). After the last major epidemic (1935-1940), sporadic cases were regularly reported from endemic states - mainly the Amazonian states - with some incursions into those of the Southeast (Minas Gerais and São Paulo, respectively in 2002 and 2008) and South (Paraná and Rio Grande do Sul in 2008), until today ( Fig. 1 ). Preceded by an upsurge of epizootics in monkeys since 2014 [ ¹1. WHO. Yellow fever in Africa and the Americas, 2016. Wkly Epidemiol Rec. 2017;92(32):442—52. ], the current epidemic resulted, from 1 December 2016 to 8 May 2018, in 2050 confirmed cases of yellow fever including 681 deaths, indicating a case fatality rate of 33.2% ( Fig. 2 ), while a further 1300 cases are still under investigation [ ²2. Brasil. Ministerio da Saude. Febre Amarela. Situação Epidemiológica/Dados. Situação Epidemiológica no Brasil. http://portalms.saude.gov.br/saude-de-a-z/febre-amarela-sintomas-transmissao-e-prevencao/situacao-epidemiologica-dados (accessed 17 Apr 2018). http://www.saude.mg.gov.br/component/search/?all=&exact=informe+epidemiol%C3%B3gico+da+febre +amarela&any=&none=&created=&modified=&area=stories (accessed 14 May 2018). https://www.paho.org/hq/index.php?option=com_topics&view= article&id=69&Itemid=40784&lang=en (accessed 14 May 2018).
http://portalms.saude.gov.br/saude-de-a-... ]. Despite a rapid and appropriate response, the epidemic spread to the east and south of the country, including areas generally considered non-endemic. This extension reproduces almost identically the course of all the epidemics observed in Brazil, including those following the reappearance of Aedes aegypti in the 1970s, after an attempt to eliminate the vector [ ³3. Mondet B, Travassos da Rosa APA, Vasconcelos PFC. Les risques d'épidémisation urbaine de la fièvre jaune au Brésil par les vecteurs de la dengue: Aedes aegypti et Aedes albopictus. Bull Soc Pathol Exot. 1996;89(2):107-13. , ⁴4. Mondet B. Epidémiologie de la fièvre jaune au Brésil. Bull Soc Pathol Exot. 2001;94(3):260-7. ]. However, in Brazil, this epidemic and the previous ones are marked by the role of wild vectors, Haemagogus sp. and Sabethes sp., involved in the sylvatic cycle, while Aedes aegypti and A. albopictus , which induce epidemics in urban and peri-urban areas, respectively [ ³3. Mondet B, Travassos da Rosa APA, Vasconcelos PFC. Les risques d'épidémisation urbaine de la fièvre jaune au Brésil par les vecteurs de la dengue: Aedes aegypti et Aedes albopictus. Bull Soc Pathol Exot. 1996;89(2):107-13. , ⁴4. Mondet B. Epidémiologie de la fièvre jaune au Brésil. Bull Soc Pathol Exot. 2001;94(3):260-7. ], do not seem to be involved in the transmission of the virus at this stage [ ²2. Brasil. Ministerio da Saude. Febre Amarela. Situação Epidemiológica/Dados. Situação Epidemiológica no Brasil. http://portalms.saude.gov.br/saude-de-a-z/febre-amarela-sintomas-transmissao-e-prevencao/situacao-epidemiologica-dados (accessed 17 Apr 2018). http://www.saude.mg.gov.br/component/search/?all=&exact=informe+epidemiol%C3%B3gico+da+febre +amarela&any=&none=&created=&modified=&area=stories (accessed 14 May 2018). https://www.paho.org/hq/index.php?option=com_topics&view= article&id=69&Itemid=40784&lang=en (accessed 14 May 2018).
http://portalms.saude.gov.br/saude-de-a-... ].

YF is an acute hemorrhagic hepatonephritis caused by an enveloped single-stranded RNA virus of approximately 12,000 base pairs belonging to the family Flavoviridae. It is transmitted by the bite of a mosquito belonging to the genus Aedes (in Africa and the Americas) or to the genera Haemagogus and Sabethes (in America). Epidemics are more frequent and important in Africa than in the Americas ( Fig. 3 ) [ ⁵5. Tomori O. Yellow fever in Africa: public health impact and prospects for control in the 21st century. Biomedica. 2002;22(2):178-210. http://www.redalyc.org/articulo.oa?id=84322213 (accessed 18 Aug 2018
http://www.redalyc.org/articulo.oa?id=84... ].

YF is native to Africa where it may have emerged around 3000 years ago [ ⁶6. Bryant JE, Holmes EC, Barrett ADT. Out of Africa: a molecular perspective on the introduction of yellow fever virus into the Americas. PLoS Pathog. 2007;3(5):e75. ]. It probably was introduced into the Americas during the beginning of the slave trade, and benefited from favorable ecological conditions, including the presence of sylvatic vectors which, although competent, forced the virus to adapt by modifying its genome to become a pathogen close to but distinct from that of Africa [ ⁷7. Mutebi JP, Rijnbrand RC, Wang H, Ryman KD, Wang E, Fulop LD, et al. Genetic relationships and evolution of genotypes of yellow fever virus and other members of the yellow fever virus group within the Flavivirus genus based on the 3’ noncoding region. J Virol. 2004;78(18):9652—65. , ⁸8. Li Y, Yang Z. Adaptive diversification between yellow fever virus west African and south American lineages: a genome-wide study. Am J Trop Med Hyg. 2017;96(3):727-34. ].

The main objective of this review is to describe the epidemiological cycles of YF in Africa and South America, particularly Brazil, and their differences. The history of YF on the two continents, and its absence from Asia, are elements that establish the conditions necessary for its maintenance and development. Recent epidemiological studies seem to indicate characteristics that might be employed to anticipate the emergence of epidemics in major Brazilian cities and improve preventive measures.

History of yellow fever and origin of the virus

YF probably impacted the history - and the economy - of Latin America more than those of Africa. Strongly linked to the development of the Americas, from its discovery by Europeans until the implementation of effective control strategies in the middle of the twentieth century, YF gave rise to strong social and political repercussions due, in particular, to the many deadly urban epidemics [ ⁹9. Patterson KD. Yellow fever epidemics and mortality in the United States, 1693-1905. Soc Sci Med. 1992;34(8):855-65. , ¹⁰10. Oldstone M. Viruses, Plagues, and history: past, present and future. New York: Oxford University Press; 2009. pp. 102-4. ]. It is certainly the recurrent YF epidemics that dissuaded Napoleon Bonaparte from achieving the conquest of the United States of America that he was preparing from then French Louisiana, with troops he had massed in the West Indies [ ¹¹11. Marr JS, Cathey JT. The 1802 saint-Domingue yellow fever epidemic and the Louisiana purchase. J Public Health Manag Pract. 2013;19(1):77-82. ]. We can also evoke the scandal of the Panama Canal, the construction of which was delayed because of an epidemic of YF [ ¹²12. Augustin G. History of yellow fever. Searcy & Pfaff ltd, New Orleans, USA; 1909. , ¹³13. Elton NW. Yellow fever in Panama; historical and contemporary. Am J Trop Med Hyg. 1952;1(3):436-56. ]. In addition, research on YF has led to conflicts between scientists because of their personal pride as well as colonialist and nationalist positions [ ¹⁴14. Delaporte F. Histoire de la fièvre jaune. Paris: Payot; 1989. ].

The history of YF entails three main controversies - now resolved - namely its mode of transmission, geographical origin and the infectious agent responsible for the disease.

The first controversy concerned the transmission of the disease and was debated throughout the nineteenth century. The theory of contagion has long prevailed [ ¹²12. Augustin G. History of yellow fever. Searcy & Pfaff ltd, New Orleans, USA; 1909. – ¹⁴14. Delaporte F. Histoire de la fièvre jaune. Paris: Payot; 1989. ]. Like the transmission of cholera, proponents of this hypothesis defended, from the seventeenth century until the end of the nineteenth century, a transmission by water and/or human contacts, then by “miasmas”. This theory - also named “aerism” - argued that the germ penetrated into the body via the respiratory system [ ¹⁵15. Lódola S, Góis Jr E. Theories about the propagation of yellow fever: the scientific debate in the São Paulo press between 1895 and 1903. Hist Cienc Saude Manguinhos 2015;22(3):687-704. http://www.scielo.br/hcsm (accessed 18 Apr 2018).
http://www.scielo.br/hcsm... ]. Changes in the concepts took place gradually between the end of the eighteenth century - after the epidemics of Philadelphia in 1793, Cadiz in 1800 and Barcelona in 1821-1822, where the lack of direct contact between the patients excluded direct contamination between people - and the demonstration of the vectorial transmission in 1900 [ ¹⁵15. Lódola S, Góis Jr E. Theories about the propagation of yellow fever: the scientific debate in the São Paulo press between 1895 and 1903. Hist Cienc Saude Manguinhos 2015;22(3):687-704. http://www.scielo.br/hcsm (accessed 18 Apr 2018).
http://www.scielo.br/hcsm... – ¹⁷17. Fournier P. Zones humides et “aérisme” à l'époque moderne. In: Derex JM, editor. Zones humides et santé. Paris: GHZH; 2010. p. 9-23. ]. The “non-contagion” was first demonstrated by several doctors in the French West Indies, notably masterfully by Lefort and his team [ ¹⁸18. Lefort P. Mémoire sur la non contagion de la fièvre jaune. Fleurot et Cie, Gouvernements de la Martinique et de Guadeloupe. 1823. ]. It was on this basis that Beauperthuy, as early as 1854, suggested the transmission of YF by mosquito, which he illustrated by protecting healthy persons with a bed net [ ¹⁹19. Beauperthuy LD. 1854. Fiebre Amarilla. Gac Ofic Cumaná. 1854;57(23 de Mayo). – ²¹21. Beauperthuy de Benedetti R. Louis Daniel Beauperthuy et la méthode scientifique, le rôle des moustiques dans la transmission de la fièvre jaune. Ann Hyg Langue Franc. 1966;2(6):25-32. ]. Following this new paradigm, Chervin proposed to abolish quarantining as the regular method for the prevention of YF [ ¹⁶16. Ackerknecht EH. Anticontagionism between 1821 and 1867. Int J Epidemiol. 2009;38(1):7-21. ]. Based on the filarial transmission model described by Manson in 1878, but without quoting the latter nor Beauperthuy, although he certainly had access to their works [ ¹⁴14. Delaporte F. Histoire de la fièvre jaune. Paris: Payot; 1989. ], Finlay [ ²²22. Finlay CJ. El mosquito hipoteticamente considerado como agente de transmisíon de la fiebre amarilla. An Acad Cienc Med Fis Nat Habana. 1881;18:147-69. ] supported the vectorial transmission of the YF that was confirmed experimentally by Reed and his team in 1900-1902 [ ²³23. Reed W. Recent researches concerning the etiology, propagation, and prevention of yellow fever, by the United States Army Commission. J Hyg (Lond). 1902;2(2):101 —19. – ²⁵25. Reed W, Carroll J, Agramonte A, Lazear JW. The etiology of yellow fever-a preliminary note. Public Health Pap Rep. 1900;26:37-53. ]. Thus, three nations claim - with varying degrees of insistence - the discovery of the vectorial transmission of YF: France, Cuba and the USA in chronological order. The merit of the American Commission, led by Reed, was having shown that the mosquito becomes infected during the first 3 days of the disease, when the viremia is sufficiently high, and that the sting contaminating the healthy subject should occur at least 12 days later to allow replication of the virus in the mosquito [ ²⁶26. Chastel C. Le centenaire de la découverte du virus de la fièvre jaune et de sa transmission par un moustique (Cuba 1900-1901). Bull Soc Pathol Exot. 2003;96(3):250-6. ], which legitimized the authorship of the discovery [ ¹⁴14. Delaporte F. Histoire de la fièvre jaune. Paris: Payot; 1989. ].

The geographical origin of YF has also long been debated. The disease was considered to have originated from the Americas, discovered at the end of the fifteenth century by the first Spanish conquerors [ ¹²12. Augustin G. History of yellow fever. Searcy & Pfaff ltd, New Orleans, USA; 1909. ]. The first description in the New World rather than in the Old one resulted from circumstantial reasons: the Americas, actual colonies for settlements and economic exploitation, attracted much more consideration than Africa, which still consisted of trading posts essentially devoted to acquiring slaves contributing to the development of the Americas. Thus, many epidemics were reported in America and the West Indies from the middle of the seventeenth century. The mention of possible or probable cases before 1647, the date of the Guadeloupe epidemic, which is generally considered the first formally identified YF epidemic in history, led to the belief that YF was already present in America at the arrival of Spanish invaders. In fact, YF would have appeared for the first time in the West Indies 2 months after the battle of La Vega-Real that Christopher Columbus launched against the Amerindians on March 24, 1495, in Hispaniola, today known as the Dominican Republic [ ²⁷27. Béranger-Féraud LJB. Traité théorique et clinique de la fièvre jaune. Paris: Doin; 1891. ]. However, the disease is mentioned under multiple names based on the very recognizable symptoms, by European navigators sailing along the African coast and the Canary Islands as early as 1494, regardless of the discovery of America [ ¹²12. Augustin G. History of yellow fever. Searcy & Pfaff ltd, New Orleans, USA; 1909. ]. It is therefore likely that the first American cases resulted from an introduction of the YF virus by the crews of Columbus between 1492 and 1495 coming from the Canary Islands where the ships of Columbus made their last resupplying before the crossing of the Atlantic Ocean.

The arguments in favor of the African origin of YF prevail and this thesis has become the consensus. The frequency of epidemics and the adaptation of the virus to its hosts and vectors argue for an older presence in Africa, which molecular biology today confirms by the greater genetic heterogeneity of the virus in Africa [ ⁷7. Mutebi JP, Rijnbrand RC, Wang H, Ryman KD, Wang E, Fulop LD, et al. Genetic relationships and evolution of genotypes of yellow fever virus and other members of the yellow fever virus group within the Flavivirus genus based on the 3’ noncoding region. J Virol. 2004;78(18):9652—65. , ²⁸28. Deubel V, Digoutte JP, Monath TP, Girard M. Genetic heterogeneity of yellow fever virus strains from Africa and the Americas. J Gen Virol. 1986; 67(Pt 1):209-13. – ³¹31. von Lindern JJ, Aroner S, Barrett ND, Wicker JA, Davis CT, Barrett AD. Genome analysis and phylogenetic relationships between east, central and west African isolates of yellow fever virus. J Gen Virol. 2006;87(Pt 4):895-907. ].

Currently, there are seven genotypes: five in Africa and two in the Americas ( Fig. 4 ). African genotypes are characterized by their affinity for their respective vectors [ ³²32. Beaty BJ, Aitken THG. In vitro transmission of yellow fever virus by geographic strains of Aedes aegypti. Mosq News. 1979;39(2):232-8. , ³³33. Ellis BR, Barrett AD. The enigma of yellow fever in East Africa. Rev Med Virol. 2008;18(5):331-46. ]. All the studies confirmed the African origin of the YF virus. The East African strain is the oldest, and probably diverged from an ancestral flavivirus about 3500 years ago [ ⁶6. Bryant JE, Holmes EC, Barrett ADT. Out of Africa: a molecular perspective on the introduction of yellow fever virus into the Americas. PLoS Pathog. 2007;3(5):e75. , ³⁴34. Monath T, Cetron MS, Teuwen DE. Yellow fever vaccine. In: Plotkin SA, Orenstein WA, Offit PA, editors. Vaccines. 5th ed. Philadelphia: Saunders Elsevier; 2008. p. 959-1055. ]. West African strains were separated from East African ones about 3 centuries before the alleged introduction of the virus into the Americas. American strains are closer to West African strains than the latter are related to the East African ones [ ⁶6. Bryant JE, Holmes EC, Barrett ADT. Out of Africa: a molecular perspective on the introduction of yellow fever virus into the Americas. PLoS Pathog. 2007;3(5):e75. , ⁷7. Mutebi JP, Rijnbrand RC, Wang H, Ryman KD, Wang E, Fulop LD, et al. Genetic relationships and evolution of genotypes of yellow fever virus and other members of the yellow fever virus group within the Flavivirus genus based on the 3’ noncoding region. J Virol. 2004;78(18):9652—65. , ³⁴34. Monath T, Cetron MS, Teuwen DE. Yellow fever vaccine. In: Plotkin SA, Orenstein WA, Offit PA, editors. Vaccines. 5th ed. Philadelphia: Saunders Elsevier; 2008. p. 959-1055. ]. The virus has encountered in the Americas a competent mosquito that allowed permanent installment of a sylvatic cycle of the virus.

However, this does not explain why the disease was never mentioned in Europe before the fifteenth century, despite numerous and intense contacts between sub-Saharan Africa - the land of YF's origin - and Europe well before the discovery of America [ ¹²12. Augustin G. History of yellow fever. Searcy & Pfaff ltd, New Orleans, USA; 1909. ]. The most likely hypothesis is the absence of a competent mosquito capable of establishing itself in a temperate zone. Subsequently, YF has been recurrent in Europe, as in North America, mainly during summer port epidemics, which are still not maintained in situ from 1 year to the next [ ²⁷27. Béranger-Féraud LJB. Traité théorique et clinique de la fièvre jaune. Paris: Doin; 1891. ]. A greater number of epidemics in the Americas from the 17th to the nineteenth century in comparison with Africa resulted from a combination of socioeconomic, demographic and ecological circumstances that favored the development of the disease in relation to Africa, where many human infections were probably limited by low population density and did not result in “conspicuous” epidemics.

While an African origin of YF is established, a new question arises: how did it cross the Atlantic Ocean? At the time of the slave trade, the duration of the journey between African and American coasts was longer than 1 month whereas the severe conditions of the crossing certainly did not favor the survival of the patients [ ³⁵35. Thomas H. The slave trade: the story of the Atlantic slave trade: 1440-1870. Touchstone, New York. 1999. Paris: French translation, Robert Lafont; 2006. ]. Incubation (3 to 6 days) and viremia (less than 10 days before the acquired immunity does not make it disappear) are too short for the virus to have been carried by slaves, if we admit the likelihood that some of them may have been infected at the time of their departure [ ³⁶36. Marchoux E, Simond PL, Salimbeni A. Etudes sur la fièvre jaune, premier mémoire. Ann Inst Pasteur. 1903;17:665-728. , ³⁷37. Nassar ES, Chamelet EL, Coimbra TL, de Souza LT, Suzuki A, Ferreira IB, et al. Jungle yellow fever: clinical and laboratorial studies emphasizing viremia on a human case. Rev Inst Med Trop Sao Paulo. 1995;37(4):337-41. ]. It is now accepted that the transfer was carried out via the mosquito Aedes aegypti , whose eggs survive for several months at desiccation [ ³⁸38. Christophers SR. Aedes aegypti (L.) the yellow fever mosquito. In: Its life history, bionomics and structure. Cambridge, Great Britain: Cambridge University Press; 1960. ], which ensures transovarial transmission of the virus [ ³⁹39. Marchoux E, Simond PL. La transmission héréditaire du virus de la fièvre jaune chez le Stegomyia fasciata. C R Soc Biol (Paris). 1905;59:259-60. – ⁴¹41. Fontenille D, Diallo M, Mondo M, Ndiaye M, Thonnon J. First evidence of natural vertical transmission of yellow fever virus in Aedes aegypti , its epidemic vector. Trans R Soc Trop Med Hyg. 1997; 91 (5):533-5. ]. The circulation of the virus and the development of the epidemics for which it is responsible are inseparable from the vectors.

Finally, the search for the pathogen has led to a long debate. Most of the works were performed in the Americas, mainly in Cuba, Brazil and Mexico, at least until the beginning of the twentieth century. This can be explained by the socioeconomic development of the Americas, particularly in the nineteenth century, the demographic changes that this region has experienced and the geopolitical influence it exerted on the world at that time. In addition, the lack of laboratories in Africa before the twentieth century did not favor research on the transmission and etiology of YF.

Brazilian scientists played a leading role. Lacerda isolated a fungus from the viscera and stool of patients [ ⁴²42. Lacerda JB. Mémoire présenté par M. de Quatrefages. Compt Rend Acad Sci. 1883;97(1):1708-9. ]. Freire discovered a Cryptococcus that he believed responsible for YF and, after culture and attenuation of the yeast virulence, he experimented to obtain a vaccine [ ⁴³43. Freire D. Doctrine microbienne de la fièvre jaune et ses inoculations préventives. Imprimerie Nationale, Rio de Janeiro. 1885. ]. In Rio de Janeiro, Havelburg found a coliform [ ⁴⁴44. Havelburg W. Recherches expérimentales et anatomiques sur la fièvre jaune. Ann Inst Pasteur. 1897;11:515-22. ], the same year that Sanarelli in Montevideo identified another bacillus from Uruguayan and Brazilian patients [ ⁴⁵45. Sanarelli J. Etiologie et pathogénie de la fièvre jaune. Ann Inst Pasteur. 1897;11(7):433-513. ]. In Cuba, Finlay and Delgado observed a bacterium, which they identified as Micrococcus tetragenus Koch and Gaffky 1881, both in the vomit of patients, proboscis of the mosquito and blood from inoculated animals [ ⁴⁶46. Finlay CJ, Delgado C. Del micrococo tetrágeno de la fiebre amarilla. Ann Acad Ciencias Med Fis Natur Habana. 1888;18:147-69. ]. The microbiologists proceeded by analogy, associating the pathogen with the seasonality of the disease, and inferring its adaptation to the environment in which it develops and/or relating the colors matching those of vomit, liver or skin.

A detailed review of potential candidates as etiological YF agents concluded that it was filterable, i.e., a pathogen not yet called a virus: “It is more than likely that the germs of yellow fever, as well as those of small pox, measles, hydrophobia, etc. belong to a group of organisms, smaller than our bacteria and as yet unknown, awaiting discovery” [ ⁴⁷47. Novy FG. The Etiology of Yellow Fever. Med News. 1898;73:326-331 and 360-9. ]. The US Mission in Cuba led by Reed has shown that the bacillus isolated by Sanarelli (Bacilus icteroides) was not the cause of YF but a secondary contaminant [ ²⁵25. Reed W, Carroll J, Agramonte A, Lazear JW. The etiology of yellow fever-a preliminary note. Public Health Pap Rep. 1900;26:37-53. ]. The French Mission in Brazil confirmed these observations and the filtering property of the YF pathogen [ ³⁶36. Marchoux E, Simond PL, Salimbeni A. Etudes sur la fièvre jaune, premier mémoire. Ann Inst Pasteur. 1903;17:665-728. ].

The YF virus was isolated June 30, 1927, from the blood of a Ghanaian patient - who recovered - by Adrian Stokes, who contracted YF and died [ ⁴⁸48. Stokes A, Bauer JH, Hudson NP. Experimental transmission of yellow fever to laboratory animals. Am J Trop Med. 1928;8:103-64. ]. The 17D vaccine - still used today - was obtained by attenuation of this strain, called Asibi after the name of the Ghanaian patient, a few years later by Theiler [ ⁴⁹49. Theiler M, Smith HH. The use of yellow fever modified by in vitro cultivation for human immunization. J Exp Med. 1937;65:787-800. ], which earned him the Nobel Prize in Medicine. A few months after the discovery by Stokes on December 21, 1927, another strain of the YF virus was isolated at the Institut Pasteur in Dakar [ ⁵⁰50. Mathis C, Sellards AW, Laigret J. Sensibilité du Macacus rhesus au virus de la fièvre jaune. C R Acad Sci. 1928;186:604-6. ], from François Miyeli a young patient from Rufisque, Senegal [ ⁵¹51. Ducloux M. François Miyeli (1911-1927 – 1973) et la souche française amarile. Bull Soc Med Afr Noire Lang Franc. 1975;20:174-9. ]. This strain was at the origin of the vaccine manufactured in Dakar (YF French Neurotropic Vaccine or FNV) [ ⁵²52. Sellards AW, Laigret J. Vaccination de l'homme contre la fièvre jaune. C R Acad Sci. 1932;194:1609-11. ]. Used throughout French-speaking Africa until 1982, the FNV was discontinued because of its adverse effects [ ⁵³53. Moreau JP, Girault G, Dramé I, Perraut R. Réémergence de la fièvre jaune en Afrique de l'Ouest: leçons du passé, plaidoyer pour un programme de contrôle. Bull Soc Pathol Exot. 1999;92(5):333-6. , ⁵⁴54. Barrett ADT. Yellow fever live attenuated vaccine: a very successful live attenuated vaccine but still we have problems controlling the disease. Vaccine. 2017;35(44):5951-5. ].

Epidemiology of yellow fever in Africa

YF has been known in Africa since the end of the fifteenth century through sporadic cases and/or limited small epidemics observed in the colonial counters of the West African coast. In East and South Africa, YF was probably rare or absent from coastal areas because of the lack of an appropriate vector.

The epidemiology of YF in West and Central Africa was well described in the 1960s to 1980s [ ⁵⁵55. Hamon J, Pichon G, Cornet M. La transmission du virus amaril en Afrique occidentale. Ecologie, répartition, fréquence et contrôle des vecteurs et observations concernant 1'épidémiologie de la fièvre jaune. Cah ORSTOM, sér Ent Med Parasitol. 1971;9(1):3-60. – ⁵⁸58. Cordellier R. L'épidémiologie de la fièvre jaune en Afrique de l'Ouest. Bull World Health Organ. 1991;69(1):73-84. ] following a long cross-section follow-up of virus circulation during and outside of epidemic periods. It is possible, schematically, to restrict the zones of virus circulation to three regions: a) the main one that harbors the endemic sylvatic cycle, i.e., the natural focus, b) a border zone of emergence, actually a latency area ensuring a transition between the latter and c) the zone of epidemics, visible part of the iceberg, made up of regions inhabited by varying densities of human populations ( Fig. 5 ).

Endemic areas are those where the virus circulates between some Aedes species, notably A. africanus and A. furcifer , and non-human primates, especially arboreal monkeys [ ⁵⁶56. Taufflieb R, Cornet M, Le Gonidec G, Robin Y. Un foyer selvatique de fièvre jaune au Sénégal oriental. Cah ORSTOM, sér Ent Med Parasitol 1973;11(3):211-220. , ⁵⁷57. Germain M, Cornet M, Mouchet J, Herve JP, Robert V, Camicas JL, et al. La fièvre jaune selvatique en Afrique: données récentes et conceptions actuelles. Med Trop (Mars). 1981;41(1):31-43. ]. In Africa, monkeys are resistant to the YF virus and, if they become infected or sick, do not die but rather become immune [ ⁵⁵55. Hamon J, Pichon G, Cornet M. La transmission du virus amaril en Afrique occidentale. Ecologie, répartition, fréquence et contrôle des vecteurs et observations concernant 1'épidémiologie de la fièvre jaune. Cah ORSTOM, sér Ent Med Parasitol. 1971;9(1):3-60. , ⁵⁹59. Hudson NP, Philip CB. Infectivity of blood during the course of experimental yellow fever. J Exp Med. 1929;50(5):553-99. ]. Humans are not present within the endemic areas and may be accidentally infected during a short forest stay, which can lead to sporadic cases and/or limited epidemics leading to the immune protection of the population and restricting the risk of local epidemics. In the zone of emergence, most often in villages bordering forest and savannah or sometimes in extensive plantations, some Aedes species, particularly A. furcifer , leave the plant coverage, penetrate the inhabited areas and bite humans that they infect [ ⁵⁸58. Cordellier R. L'épidémiologie de la fièvre jaune en Afrique de l'Ouest. Bull World Health Organ. 1991;69(1):73-84. ].

The endemic zone tends to spread, partly because of the transovarial transmission of YF in mosquitos [ ³⁹39. Marchoux E, Simond PL. La transmission héréditaire du virus de la fièvre jaune chez le Stegomyia fasciata. C R Soc Biol (Paris). 1905;59:259-60. – ⁴¹41. Fontenille D, Diallo M, Mondo M, Ndiaye M, Thonnon J. First evidence of natural vertical transmission of yellow fever virus in Aedes aegypti , its epidemic vector. Trans R Soc Trop Med Hyg. 1997; 91 (5):533-5. ] and, secondly, because of the anthropization of the environment due to deforestation and population growth. Global warming could play an increasing role in the near future by changing environmental conditions to favor the vectors, in particular through alterations in the rain regime.

In-depth studies of viral infection in wild mammals and specific antibodies showed that vertebrates in general, including monkeys, play only a secondary role in the persistence and resilience of the virus in the sylvatic cycle, because of the short duration of viremia and the resulting definitive immunity, which reflects an effective adaptation of the virus to its transient host [ ⁵⁶56. Taufflieb R, Cornet M, Le Gonidec G, Robin Y. Un foyer selvatique de fièvre jaune au Sénégal oriental. Cah ORSTOM, sér Ent Med Parasitol 1973;11(3):211-220. , ⁵⁷57. Germain M, Cornet M, Mouchet J, Herve JP, Robert V, Camicas JL, et al. La fièvre jaune selvatique en Afrique: données récentes et conceptions actuelles. Med Trop (Mars). 1981;41(1):31-43. , ⁶⁰60. Chippaux-Hyppolite C, Chippaux A. Etude du réservoir animal dans le cycle de quelques arbovirus en Afrique centrale. I. Etude immunologique chez divers animaux domestiques et sauvages. Bull Soc Pathol Exot. 1969;62(6):1034-45. – ⁶²62. Taufflieb R, Robin Y, Cornet M. Le virus amaril et la faune sauvage en Afrique. Cah ORSTOM. 1971;9(4):351-71. ]. Humans are no exception to this rule, whether they live in primary forest like the Pygmies of Central Africa or in villages close to natural foci, although their susceptibility to infection is probably higher [ ⁶³63. Chippaux A, Chippaux-Hyppolite C. Immunologie des arbovirus chez des pygmées Babinga en République Centrafrique. Bull Soc Pathol Exot. 1965;58(5):820-33. , ⁶⁴64. Chippaux-Hyppolite C, Chippaux A. Les anticorps antiamarils chez les enfants en République centrafricaine. Bull World Health Organ. 1966; 34(1):105-11. ]. Wild vertebrates, no more than humans, cannot be considered a virus reservoir, a function that has essentially devolved to mosquitoes through the transovarial transmission of the virus. During estivation, the virus is maintained in the eggs of Aedes , thereby ensuring infection of the adults at their hatching at the beginning of the following season. On the other hand, monkeys - and possibly other small mammals -, especially the young still immunologically naive ones, amplify, reveal and propagate the virus from the first rains, thus perpetuating the sylvatic cycle [ ⁵⁷57. Germain M, Cornet M, Mouchet J, Herve JP, Robert V, Camicas JL, et al. La fièvre jaune selvatique en Afrique: données récentes et conceptions actuelles. Med Trop (Mars). 1981;41(1):31-43. ].

In the epidemic zone, the virus does not circulate and the wild vector does not occur. The population shows a low immune status, except in immunized individuals, which in case of low immunization coverage explains the intensity of the epidemic [ ⁵³53. Moreau JP, Girault G, Dramé I, Perraut R. Réémergence de la fièvre jaune en Afrique de l'Ouest: leçons du passé, plaidoyer pour un programme de contrôle. Bull Soc Pathol Exot. 1999;92(5):333-6. ]. In urban and peri-urban areas, YF transmission is ensured by other Aedes species, first of all A. aegypti. The virus is spread in the municipality, amplified by the proliferation of A. aegypti , where there are favorable conditions, lack of immunity among a large proportion of the inhabitants and, even today, health-system insufficiency based on the tripartite approach: mass vaccination, vector control, screening and treatment of cases placed under bed nets.

YF vaccination was made mandatory in 1941 in all French-controlled colonies. Facilitated by its stability and administration by scarification associated with the smallpox vaccine, mass immunization led to remarkably effective control of YF [ ⁵5. Tomori O. Yellow fever in Africa: public health impact and prospects for control in the 21st century. Biomedica. 2002;22(2):178-210. http://www.redalyc.org/articulo.oa?id=84322213 (accessed 18 Aug 2018
http://www.redalyc.org/articulo.oa?id=84... , ⁵³53. Moreau JP, Girault G, Dramé I, Perraut R. Réémergence de la fièvre jaune en Afrique de l'Ouest: leçons du passé, plaidoyer pour un programme de contrôle. Bull Soc Pathol Exot. 1999;92(5):333-6. ]. Its use was suspended in 1960 in children under 10 years because of the risk of serious adverse effects related to the use of the FNV manufactured in Dakar - although no case had been reported in a dozen years - then definitively interrupted in 1980. The disease reappeared and grew from 1965 in almost all French-speaking countries of sub-Saharan Africa. Since the late 1990s, in the face of renewed outbreaks of YF throughout Africa, sub-Saharan countries are progressively including the more tolerable 17D vaccine in the Expanded Program on Immunization by introducing routine YF vaccination in 9-month-old children together with the measles immunization supported by GAVI (Global Alliance for Vaccines and Immunization).

Epidemiology of yellow fever in the Americas

In South America, YF was mentioned at the same time as in Africa and in similar circumstances - during the slave trade - first in the Caribbean and in Central America (Yucatan).

In Brazil, the first indisputable description of YF was made after the Pernambuco epidemic in Recife and Olinda in 1685 [ ⁶⁵65. Rosa JF. Tratado Único da Constituição Pestilencial de Pernambuco. Pernambuco - Brasil 1694. http://objdigital.bn.br/objdigital2/acervo_digital/div_manuscritos/mss1428710/mss1428710.pdf. Accessed 17 Aug 2018.
http://objdigital.bn.br/objdigital2/acer... ]. Legend has it that a boat from the Cape Verde Islands carried slaves with an unknown disease [ ⁶⁶66. Franco O. História da Febre-Amarela no Brasil. Rio de Janeiro: Ministério da Saúde; 1969. ]. In fact, the boat had stopped in Guadeloupe, where YF was endemic if not epidemic [ ²⁷27. Béranger-Féraud LJB. Traité théorique et clinique de la fièvre jaune. Paris: Doin; 1891. ], before reaching the Brazilian coast [ ⁶⁷67. dos Anjos BC. Single treaty on the pestilential constitution of Pernambuco: first description of the “males” by João Ferreira da Rosa in the XVII century. Tempo. 2016;8(1):11 —36. ]. It is also possible that Cape Verdean mosquitoes, and not Antillean patients, introduced the virus into Pernambuco. However, the infection of passengers by YF was refuted by Gouy [ ⁶⁸68. Gouy E. Histoire de la fièvre jaune au Brésil. Paris: Alfonse Dorenne; 1884. ] who diagnosed food poisoning by the spoiled meats consumed during the trip based on the kinetics and symptoms of the disease.

Anyway, the penetration of YF in America via Brazil is not excluded because of the considerable economic development of Brazil starting from 1554. The expansion of sugar plantations was favored by the large spaces available and the tax benefits granted by Portugal. On the one hand, the need for labor not met by indigenous natives was assumed by the massive influx of African slaves (3500 individuals per year on average at the end of the sixteenth century). On the other hand, the crossing from Africa to Brazil was shorter than that to the West Indies or North America due to the proximity of both coasts and favorable winds, resulting in the multiplication of YF transport opportunities [ ³⁵35. Thomas H. The slave trade: the story of the Atlantic slave trade: 1440-1870. Touchstone, New York. 1999. Paris: French translation, Robert Lafont; 2006. , ⁶⁹69. McNeill JR. Yellow Jack and Geopolitics: environment, epidemics, and the struggles for empire in the american tropics, 1650-1825. OAH Mag Hist. 2004;18(3):9—13. , ⁷⁰70. Pétré-Grenouilleau O. Les Traites négrières. Essai d'histoire globale. Gallimard coll. « Bibliothèque des Histoires », Paris; 2004. p. 201-5. ]. In addition, the agricultural techniques favored the development of A. aegypti ensuring the perpetuation and dispersal of the virus [ ⁶⁹69. McNeill JR. Yellow Jack and Geopolitics: environment, epidemics, and the struggles for empire in the american tropics, 1650-1825. OAH Mag Hist. 2004;18(3):9—13. ]. YF was reported in the ports of Pernambuco in 1640 and, perhaps, in other regions of Brazil [ ²⁷27. Béranger-Féraud LJB. Traité théorique et clinique de la fièvre jaune. Paris: Doin; 1891. , ⁶⁶66. Franco O. História da Febre-Amarela no Brasil. Rio de Janeiro: Ministério da Saúde; 1969. ]. It is therefore conceivable that the YF virus had been already endemic in Brazil since the sixteenth century and that the epidemic resulted from an indigenous strain emergence.

The endemic zone of YF is located in the Amazon and encompasses, to the west, Peru and Colombia, to the north the Guyana plateau (Venezuela, Guyana, Surinam and French Guiana), and to the northeast, Brazil. The description of the sylvatic cycle was made on the occasion of the great 1942 epidemic in Brazil [ ⁷¹71. Taylor RM, Fonseca da Cunha J. An epidemiological study of jungle yellow fever in an endemic area in Brazil; epidemiology of human infections; investigation of vertebrate hosts and arthropod vectors. Am J Trop Med Hyg. 1946;26(6 Suppl 2):69. , ⁷²72. Laemmert HW Jr, Ferreira LC, Taylor RM. An epidemiological study of jungle yellow fever in an endemic area in Brazil. Investigation of vertebrate hosts and arthropod vectors. Am J Trop Med Hyg. 1946;26(6 Suppl 2):23-69. ]. The circulation of the virus seems persistent, even if the detailed mechanisms were not yet discovered [ ⁷³73. Moreira-Soto A, Torres MC, Lima de Mendonça MC, Mares-Guia MA, Dos Santos Rodrigues CD, Fabri AA, et al. Evidence for multiple sylvatic transmission cycles during the 2016-2017 yellow fever virus outbreak, Brazil. Clin Microbiol Infect. 2018; ]. It is notable, for example, that specific immunity is maintained in monkeys from many parts of Brazil, even outside the Amazon, regardless of epidemic episodes, suggesting a regular infection of the monkeys by the virus resulting in a lasting immunization in survivors [ ⁷⁴74. Kumm HW, Laemmert HW Jr. The geographical distribution of immunity to yellow fever among the primates of Brazil. Am J Trop Med Hyg. 1950;30(5):733-48. ]. While the general pattern remains fairly similar to the African one ( Fig. 5 ), there are some important differences. First, the American monkey is susceptible to the YF virus and many individuals die from it [ ⁷⁵75. Davis NC, Shannon RC. Studies on south American yellow fever: iii. Transmission of the virus to Brazilian monkeys preliminary observations. J Exp Med. 1929;50(1):81-5. ]. Thus, it not only plays the role of amplifying YF endemia as in Africa [ ⁷³73. Moreira-Soto A, Torres MC, Lima de Mendonça MC, Mares-Guia MA, Dos Santos Rodrigues CD, Fabri AA, et al. Evidence for multiple sylvatic transmission cycles during the 2016-2017 yellow fever virus outbreak, Brazil. Clin Microbiol Infect. 2018; ] but also reveals the risk of epidemics: periodic epizootics that occur near inhabited regions are used as a warning signal [ ⁷⁶76. Fernandes NCCA, Cunha MS, Guerra JM, Réssio RA, Cirqueira CDS, Iglezias SD, et al. Outbreak of yellow fever among nonhuman primates, Espirito Santo, Brazil, 2017. Emerg Infect Dis. 2017;23(12):2038-41. ]. In addition, the vectors are different - at least within the jungle cycle - in which Haemagogus janthinomys and H. leucocelaenus play an essential role while other species (including H. capricornii) or genera, notably Aedes , are little involved in the transmission [ ⁷²72. Laemmert HW Jr, Ferreira LC, Taylor RM. An epidemiological study of jungle yellow fever in an endemic area in Brazil. Investigation of vertebrate hosts and arthropod vectors. Am J Trop Med Hyg. 1946;26(6 Suppl 2):23-69. , ⁷⁷77. Pajot FX, Geoffroy B, Chippaux JP. Écologie d'Haemagogus, janthinomys Dyar (Diptera, Culicidae) en Guyane française. Cah ORSTOM. 1985;23(3):209-16. – ⁸³83. Mucci LF, Medeiros-Sousa AR, Ceretti-Júnior W, Fernandes A, Camargo AA, Evangelista E, et al. Haemagogus leucocelaenus and other mosquitoes potentially associated with sylvatic yellow fever in Cantareira State Park in the São Paulo metropolitan area, Brazil. J Am Mosq Control Assoc. 2016;32(4):329-32. ]. On the other hand, A. aegypti and A. albopictus represent a major risk of spreading YF in urban and peri-urban areas [ ⁸⁴84. Couto-Lima D, Madec Y, Bersot MI, Campos SS, Motta MA, Santos FBD, et al. Potential risk of re-emergence of urban transmission of yellow fever virus in Brazil facilitated by competent Aedes populations. Sci Rep. 2017;7(1):4848. ].

Despite common ecological conditions in the Amazonian region, there are two lineages of the YF virus: genotype 1 from Brazil (or possibly from the West Indies) and genotype 2 from Peru [ ⁶6. Bryant JE, Holmes EC, Barrett ADT. Out of Africa: a molecular perspective on the introduction of yellow fever virus into the Americas. PLoS Pathog. 2007;3(5):e75. , ⁸⁵85. Vasconcelos PFC, Bryant JE, da Rosa APAT, Tesh RB, Rodrigues SG, Barrett ADT. Genetic divergence and dispersal of yellow fever virus, Brazil. Emerg Infect Dis. 2004;10(9):1578-84. – ⁸⁷87. Carrington CV, Auguste AJ. Evolutionary and ecological factors underlying the tempo and distribution of yellow fever virus activity. Infect Genet Evol. 2013;13:198-210. ]. A strong genetic heterogeneity of the virus has been developing for some 30 years, increasing since the 2000s, probably as a result of human migrations that play a role of both gene mixing and viral dispersal [ ⁸⁵85. Vasconcelos PFC, Bryant JE, da Rosa APAT, Tesh RB, Rodrigues SG, Barrett ADT. Genetic divergence and dispersal of yellow fever virus, Brazil. Emerg Infect Dis. 2004;10(9):1578-84. , ⁸⁸88. de Souza RP, Foster PG, Sallum MA, Coimbra TL, Maeda AY, Silveira VR, et al. Detection of a new yellow fever virus lineage within the south American genotype I in Brazil. J Med Virol. 2010;82(1):175-85. , ⁸⁹89. Mir D, Delatorre E, Bonaldo M, Lourenço-de-Oliveira R, Vicente AC, Bello G. Phylodynamics of yellow fever virus in the Americas: new insights into the origin of the 2017 Brazilian outbreak. Sci Rep. 2017; 7(1):7385. ].

The reemergence of YF in Brazil benefits from particularly favorable environmental conditions: high deforestation increasing the contact of human populations with the sylvatic virus, substantial migration between endemic and epidemic regions, poorly controlled urbanization favoring the multiplication of vectors, low immunization coverage in epidemic risk areas [ ⁹⁰90. Vasconcelos PF, Rodrigues SG, Degallier N, Moraes MA, da Rosa JF, da Rosa ES, et al. An epidemic of sylvatic yellow fever in the southeast region of Maranhao state, Brazil, 1993-1994: epidemiologic and entomologic findings. Am J Trop Med Hyg. 1997;57(2):132-7. ]. Finally, the role of the recent dengue and Zika epidemics, transmission of which is ensured by the same vectors, in diverting attention and /or complicating the logistics of the health services, remains to be elucidated.

On the occasion of the Rio de Janeiro epidemic of 1900, the French scientific mission demonstrated the vertical transmission of the pathogen in mosquitos, and identified the former as small filtering organism. The first vaccine trials were undertaken [ ³⁶36. Marchoux E, Simond PL, Salimbeni A. Etudes sur la fièvre jaune, premier mémoire. Ann Inst Pasteur. 1903;17:665-728. , ³⁹39. Marchoux E, Simond PL. La transmission héréditaire du virus de la fièvre jaune chez le Stegomyia fasciata. C R Soc Biol (Paris). 1905;59:259-60. , ⁴⁰40. Marchoux E, Simond PL. Etudes sur la fièvre jaune, deuxième mémoire. Ann Inst Pasteur. 1906;25:16-40. ]. At the end of the mission, new health measures produced spectacular results.

The control of A. aegypti started in the 1920s in most Latin American countries, reinforced by the use of DDT from 1947 [ ⁹¹91. Severo OP. Eradication of the Aedes aegypti Mosquito from the Americas. In “Yellow fever, a symposium in commemoration of Carlos Juan Finlay, 1955. Paper 6. http://jdcjefferson.edu/yellow_fever_symposium/6 (accessed 14 May 2018).
http://jdcjefferson.edu/yellow_fever_sym... ]. Mass vaccination campaigns started after the discovery of the 17D vaccine in 1937. The elimination of the vector and immunization of a large part of the Brazilian population were considered major public health achievements and established an expectation of YF elimination in Brazil and perhaps more widely in Latin America. The persistence of the sylvatic transmission of YF, or “jungle cycle”, and resurgence of A. aegypti from jungle foci were unexpected [ ⁷³73. Moreira-Soto A, Torres MC, Lima de Mendonça MC, Mares-Guia MA, Dos Santos Rodrigues CD, Fabri AA, et al. Evidence for multiple sylvatic transmission cycles during the 2016-2017 yellow fever virus outbreak, Brazil. Clin Microbiol Infect. 2018; , ⁹²92. Kotsakiozi P, Gloria-Soria A, Caccone A, Evans B, Schama R, Martins AJ, et al. Tracking the return of Aedes aegypti to Brazil, the major vector of the dengue, chikungunya and Zika viruses. PLoS Negl Trop Dis. 2017;11 (7):e0005653. ].

The role of the vector and its cooperation with the virus

The YF virus and its vector live in close symbiosis in which the evolution of the former seems irremediably linked to that of the latter. The virus-vector coadaptation is essential for maintaining the sylvatic cycle. This is the case in Africa and South America where the virus adapted to various species of Culicidae in forest areas that have become endemic. Humans become infected and spread the epidemic all the more rapidly so that, on the one hand, the mosquito is both receptive to the virus and anthropophilic, which is the case for A. aegypti and A. albopictus and, on the other hand, the human population lacks herd immunity.

These two species, in particular A. aegypti , favor the transport of the virus because of the resistance of their eggs to the desiccation [ ⁹³93. Reiter P. Aedes albopictus and the world trade in used tires, 1988-1995: the shape of things to come? J Am Mosq Control Assoc. 1998;14(1):83-94. ] that leads to the resilience of the YF virus [ ⁹⁴94. Diallo M, Thonnon J, Fontenille D. Vertical transmission of the yellow fever virus by Aedes aegypti (Diptera, Culicidae): dynamics of infection in F1 adult progeny of orally infected females. Am J Trop Med Hyg. 2000;62(1):151-6. , ⁹⁵95. Díaz-Nieto LM, Chiappero MB, Díaz de Astarloa C, Maciá A, Gardenal CN, Berón CM. Genetic evidence of expansion by passive transport of Aedes (Stegomyia) aegypti in eastern Argentina. PLoS Negl Trop Dis. 2016;10(9):e0004839. ]. The spread of YF probably occurred at the same time as that of A. aegypti . The short flying distance of Aedes , especially A. aegypti and A. albopictus , leaves no alternative other than passive transport, especially by the transportation of humans or goods [ ⁹⁶96. Trpis M, Hausermann W. Dispersal and other population parameters of Aedes aegypti in an African village and their possible significance in epidemiology of vector-borne diseases. Am J Trop Med Hyg. 1986; 35(6):1263-79. – ¹⁰²102. Guagliardo SA, Barboza JL, Morrison AC, Astete H, Vazquez-Prokopec G, Kitron U. Patterns of geographic expansion of Aedes aegypti in the Peruvian Amazon. PLoS Negl Trop Dis. 2014;8(8):e3033. ].

The molecular phylogeny of A. aegypti strains confirmed the African origin of the species although genetic variability reflected massive mixings due to multiple importations over time from all continents, and human intervention for controlling mosquitoes [ ¹⁰³103. Mousson L, Dauga C, Garrigues T, Schaffner F, Vazeille M, Failloux AB. Phylogeography of Aedes ( Stegomyia ) aegypti (L.) and Aedes ( Stegomyia ) albopictus (Skuse) (Diptera: Culicidae) based on mitochondrial DNA variations. Genet Res. 2005;86(1):1-11. , ¹⁰⁴104. Moore M, Sylla M, Goss L, Burugu MW, Sang R, Kamau LW, et al. Dual African origins of global Aedes aegypti s.L. populations revealed by mitochondrial DNA. PLoS Negl Trop Dis. 2013;7(4):e2175. ]. In addition, genetic heterogeneity resulted in a high variability in susceptibility to viral infection according to vector strains [ ¹⁰⁵105. Tabachnick WJ, Wallis GP, Aitken TH, Miller BR, Amato GD, Lorenz L, et al. Oral infection of Aedes aegypti with yellow fever virus: geographic variation and genetic considerations. Am J Trop Med Hyg. 1985;34(6):1219-24. – ¹⁰⁸108. Tabachnick WJ. Nature, nurture and evolution of intra-species variation in mosquito arbovirus transmission competence. Int J Environ Res Public Health. 2013;10(1):249-77. ]. The original strain - now known as A. aegypti formosus as opposed to the subspecies A. aegypti aegypti , which is the domestic and urban form of the species - is still present in African jungle where the larvae grow in tree trunks, and whose females are not anthropophilic [ ¹⁰⁹109. Brown JE, McBride CS, Johnson P, Ritchie S, Paupy C, Bossin H, et al. Worldwide patterns of genetic differentiation imply multiple ‘domestications’ of Aedes aegypti , a major vector of human diseases. Proc Biol Sci. 2011;278(1 717):2446-54. – ¹¹¹111. Powell JR, Tabachnick WJ. History of domestication and spread of Aedes aegypti - a review. Mem Inst Oswaldo Cruz. 2013;108(Suppl 1):11 —7. ]. A. aegypti formosus is involved in the transmission of YF in nonhuman primates within the sylvatic cycle [ ¹¹²112. Crawford JE, Alves JM, Palmer WJ, Day JP, Sylla M, Ramasamy R, et al. Population genomics reveals that an anthropophilic population of Aedes aegypti mosquitoes in West Africa recently gave rise to American and Asian populations of this major disease vector. BMC Biol. 2017;15(1):16. ]. It is not known whether the domestication of A. aegypti , which led to its diffusion in America, was earlier or contemporaneous with its transport during the slave trade [ ¹¹¹111. Powell JR, Tabachnick WJ. History of domestication and spread of Aedes aegypti - a review. Mem Inst Oswaldo Cruz. 2013;108(Suppl 1):11 —7. ]. In either scenario, A. aegypti adaptation to human populations in West Africa was early, which explains the many large urban epidemics in this part of the continent at the end of the eighteenth century [ ²⁷27. Béranger-Féraud LJB. Traité théorique et clinique de la fièvre jaune. Paris: Doin; 1891. ]. On the other hand, in East Africa, A. aegypti does not seem to have adapted to the anthropization of the environment, as evidenced by the scarcity of urban epidemics up to the present day [ ¹¹³113. Mutebi JP, Barrett AD. The epidemiology of yellow fever in Africa. Microbes Infect. 2002;4(14):1459-68. ].

The colonization of Asia by A. aegypti was later, probably at the end of the nineteenth century when it was revealed as an urban vector of dengue fever [ ¹¹⁴114. Smith CE. The history of dengue in tropical Asia and its probable relationship to the mosquito Aedes aegypti. J Trop Med Hyg. 1956;59(10):243—51. ]. Phylogenetic data suggest that the Asian strain originates from the Americas and not from East Africa as might have been expected, probably because of the poor adaptation of the East African strain to humans and its poor susceptibility to the YF virus [ ³³33. Ellis BR, Barrett AD. The enigma of yellow fever in East Africa. Rev Med Virol. 2008;18(5):331-46. , ¹⁰⁸108. Tabachnick WJ. Nature, nurture and evolution of intra-species variation in mosquito arbovirus transmission competence. Int J Environ Res Public Health. 2013;10(1):249-77. , ¹¹¹111. Powell JR, Tabachnick WJ. History of domestication and spread of Aedes aegypti - a review. Mem Inst Oswaldo Cruz. 2013;108(Suppl 1):11 —7. ]. In addition, the genetic homogeneity of Asian strains of A. aegypti suggests that the introduction was recent and accomplished by a limited number of entries [ ¹¹⁵115. Wallis GP, Tabachnick WJ, Powell JR. Macrogeographic genetic variation in a human commensal: Aedes aegypti , the yellow fever mosquito. Genet Res. 1983;41(3):241 —58. ]. However, although the current strain of A. aegypti aegypti is monophyletic [ ¹¹⁰110. Brown JE, Evans BR, Zheng W, Obas V, Barrera-Martinez L, Egizi A, et al. Human impacts have shaped historical and recent evolution in Aedes aegypti , the dengue and yellow fever mosquito. Evolution. 2014;68(2):514-25. ], it has important local polymorphisms [ ¹¹⁶116. Scarpassa VM, Cardoza TB, Cardoso Junior RP. Population genetics and phylogeography of Aedes aegypti (Diptera: Culicidae) from Brazil. Am J Trop Med Hyg. 2008;78(6):895-903. , ¹¹⁷117. Louise C, Vidal PO, Suesdek L. Microevolution of Aedes aegypti. PLoS One. 2015;10(9):e0137851. ] that could explain, at least in part, the variability of the vector competence [ ³²32. Beaty BJ, Aitken THG. In vitro transmission of yellow fever virus by geographic strains of Aedes aegypti. Mosq News. 1979;39(2):232-8. , ¹⁰⁵105. Tabachnick WJ, Wallis GP, Aitken TH, Miller BR, Amato GD, Lorenz L, et al. Oral infection of Aedes aegypti with yellow fever virus: geographic variation and genetic considerations. Am J Trop Med Hyg. 1985;34(6):1219-24. , ¹⁰⁷107. Bernhardt SA, Simmons MP, Olson KE, Beaty BJ, Blair CD, Black WC. Rapid intraspecific evolution of miRNA and siRNA genes in the mosquito Aedes aegypti. PLoS One. 2012;7(9):e44198. , ¹¹⁸118. Black WC 4th, Bennett KE, Gorrochótegui-Escalante N, Barillas-Mury CV, Fernández-Salas I, de Lourdes Munoz M, et al. Flavivirus susceptibility in Aedes aegypti. Arch Med Res. 2002;33(4):379-88. ].

Absence of the YF from Asia and Oceania

The absence of YF from Asia and Oceania remains an enigma. The population is susceptible to the virus as shown by Asian patients living in endemic areas (Africa or South America). A. aegypti , although a recent arrival, is present in many places in Asia and Oceania. In addition, the abundant circulation of other arboviruses, dengue, chikungunya and Zika, the latter two coming from Africa like YF, indicates the possibility of YF extension in Asia. Recently, several human cases of YF introduced from Angola have been diagnosed in China [ ¹¹⁹119. Cui S, Pan Y, Lyu Y, Liang Z, Li J, Sun Y, et al. Detection of yellow fever virus genomes from four imported cases in China. Int J Infect Dis. 2017;60:93-5. ], increasing YF outbreak fears. Several studies attempted to explain the absence of YF in Asia. The following main reasons were given: a) poor competency of the vector for the virus [ ³²32. Beaty BJ, Aitken THG. In vitro transmission of yellow fever virus by geographic strains of Aedes aegypti. Mosq News. 1979;39(2):232-8. , ¹⁰⁵105. Tabachnick WJ, Wallis GP, Aitken TH, Miller BR, Amato GD, Lorenz L, et al. Oral infection of Aedes aegypti with yellow fever virus: geographic variation and genetic considerations. Am J Trop Med Hyg. 1985;34(6):1219-24. , ¹⁰⁸108. Tabachnick WJ. Nature, nurture and evolution of intra-species variation in mosquito arbovirus transmission competence. Int J Environ Res Public Health. 2013;10(1):249-77. , ¹¹⁸118. Black WC 4th, Bennett KE, Gorrochótegui-Escalante N, Barillas-Mury CV, Fernández-Salas I, de Lourdes Munoz M, et al. Flavivirus susceptibility in Aedes aegypti. Arch Med Res. 2002;33(4):379-88. ], b) poor adaptation of the vector to humans and competition between vectors (Abrão and Fonseca, 2006, quoted in [ ¹²⁰120. Wasserman S, Tambyah PA, Lim PL. Yellow fever cases in Asia: primed for an epidemic. Int J Infect Dis. 2016;48:98-103. ]), c) competition between Flavoviridae in the vector at the expense of YF and d) cross-reactivity with other Flavoviridae, including dengue fever, in humans and other animals [ ¹²¹121. Theiler M, Anderson CR. The relative resistance of dengue-immune monkeys to yellow fever virus. Am J Trop Med Hyg. 1975;24(1):115-7. , ¹²²122. Xiao SY, Guzman H, da Rosa AP, Zhu HB, Tesh RB. Alteration of clinical outcome and histopathology of yellow fever virus infection in a hamster model by previous infection with heterologous flaviviruses. Am J Trop Med Hyg. 2003;68(6):695-703. ]. Recent modeling of YF risk in Asia showed that two major factors limited the probability of YF expansion in Asia (“Asian hypothesis”) and dengue fever in Africa (“African hypothesis”) [ ¹²³123. Amaku M, Coutinho FA, Massad E. Why dengue and yellow fever coexist in some areas of the world and not in others? Biosystems. 2011;106(2-3):111-20. ]. The first was based on cross-immunity between Flavoviridae - especially between dengue and YF, which could limit the risk of double infection - and high viremia and severe clinical forms of YF [ ¹²¹121. Theiler M, Anderson CR. The relative resistance of dengue-immune monkeys to yellow fever virus. Am J Trop Med Hyg. 1975;24(1):115-7. , ¹²²122. Xiao SY, Guzman H, da Rosa AP, Zhu HB, Tesh RB. Alteration of clinical outcome and histopathology of yellow fever virus infection in a hamster model by previous infection with heterologous flaviviruses. Am J Trop Med Hyg. 2003;68(6):695-703. ]. The second was based on the competition between A. aegypti and A. albopictus as well as on their respective competencies in the transmission of dengue and YF to explain the absence of the latter in Asia and the rarity of the former in Africa [ ¹²⁰120. Wasserman S, Tambyah PA, Lim PL. Yellow fever cases in Asia: primed for an epidemic. Int J Infect Dis. 2016;48:98-103. ]. Another explanation was the low probability of transporting the virus from Africa - or the Americas - to Asia and the Pacific. The slave trade to Asia was much smaller than the trade to the Americas. This reduces the probability - as to the transport of the virus into the Americas before air transport - by infected humans [ ¹²⁴124. Cathey JT, Marr JS. Yellow fever, Asia and the east African slave trade. Trans R Soc Trop Med Hyg. 2014;108(5):252-7. ]. Mosquito transport did not occur, either from Africa or America, for reasons that have not yet been elucidated.

Rooting out and controlling of yellow fever in Brazil

Since its introduction in the seventeenth century, YF remained in the Amazonian region in the form of a jungle cycle that causes rural, peri-urban or urban epidemics at regular intervals. The sylvatic cycle is maintained by wild endemic vectors present before the introduction of YF in Brazil - belonging to the genera Haemagogus and Sabethes - playing the role of virus reservoir, especially in the Amazon that is the refuge zone of the virus [ ³3. Mondet B, Travassos da Rosa APA, Vasconcelos PFC. Les risques d'épidémisation urbaine de la fièvre jaune au Brésil par les vecteurs de la dengue: Aedes aegypti et Aedes albopictus. Bull Soc Pathol Exot. 1996;89(2):107-13. , ⁷⁹79. Mondet B, Vasconcelos PF, Travassos da Rosa AP, Travassos da Rosa ES, Rodrigues SG, Travassos Rosa JF, et al. Isolation of yellow fever virus from nulliparous Haemagogus ( Haemagogus ) janthinomys in eastern Amazonia. Vector Borne Zoonotic Dis. 2002;2(1):47-50. – ⁸³83. Mucci LF, Medeiros-Sousa AR, Ceretti-Júnior W, Fernandes A, Camargo AA, Evangelista E, et al. Haemagogus leucocelaenus and other mosquitoes potentially associated with sylvatic yellow fever in Cantareira State Park in the São Paulo metropolitan area, Brazil. J Am Mosq Control Assoc. 2016;32(4):329-32. ]. Extension to peri-urban and urban areas involves A. albopictus and A. aegypti respectively, and follows the routes of human migrations, particularly forest galleries [ ⁴4. Mondet B. Epidémiologie de la fièvre jaune au Brésil. Bull Soc Pathol Exot. 2001;94(3):260-7. ].

Clinically, the Brazilian YF does not differ from the forms described in Africa or other American countries. The high case fatality rate (up to 50%) is likely not to be the manifestation of a particular virulence but resulted from underreporting of benign cases [ ¹²⁵125. Tuboi SH, Costa ZG, Vasconcelos PF, Hatch D. Clinical and epidemiological characteristics of yellow fever in Brazil: analysis of reported cases 1998-2002. Trans R Soc Trop Med Hyg. 2007;101(2):169-75. ].

The vector control carried out at the beginning of the twentieth century during the Rio de Janeiro epidemic was organized nationwide in 1928-29. It was reinforced by YF immunization in 1937 and DDT sprayings initiated 10 years later, which significantly reduced the burden of YF, that was considered as having been eliminated from Brazil in the 60s [ ⁹¹91. Severo OP. Eradication of the Aedes aegypti Mosquito from the Americas. In “Yellow fever, a symposium in commemoration of Carlos Juan Finlay, 1955. Paper 6. http://jdcjefferson.edu/yellow_fever_symposium/6 (accessed 14 May 2018).
http://jdcjefferson.edu/yellow_fever_sym... , ¹²⁶126. Wermelinger ED, Carvalho RW. Methods and procedures used in Aedes aegypti control in the successful campaign for yellow fever prophylaxis in Rio de Janeiro, Brazil, in 1928 and 1929. Epidemiol Serv Saude. 2016;25(4):837-44. ]. However, the epidemics of dengue in 1963-64 then in 1968-69 marked the beginning of the re-infestation of the continent by A. aegypti , confirmed between 1971 and 1999 [ ¹²⁷127. Brathwaite Dick O, San Martín JL, Montoya RH, del Diego J, Zambrano B, Dayan GH. The history of dengue outbreaks in the Americas. Am J Trop Med Hyg. 2012;87(4):584-93. ], which resulted in the return of YF and, more recently, the installation of other arboviruses (chikungunya and Zika, in particular) [ ²2. Brasil. Ministerio da Saude. Febre Amarela. Situação Epidemiológica/Dados. Situação Epidemiológica no Brasil. http://portalms.saude.gov.br/saude-de-a-z/febre-amarela-sintomas-transmissao-e-prevencao/situacao-epidemiologica-dados (accessed 17 Apr 2018). http://www.saude.mg.gov.br/component/search/?all=&exact=informe+epidemiol%C3%B3gico+da+febre +amarela&any=&none=&created=&modified=&area=stories (accessed 14 May 2018). https://www.paho.org/hq/index.php?option=com_topics&view= article&id=69&Itemid=40784&lang=en (accessed 14 May 2018).
http://portalms.saude.gov.br/saude-de-a-... ]. Several factors can explain this phenomenon. The most important is, almost certainly the reinvasion of A. aegypti from isolated and poorly controlled Amazonian and Southern Brazilian forest localities, as a result of a relaxation of vector control and vaccination campaigns, as well as the deterioration of health systems in some remote areas [ ⁹²92. Kotsakiozi P, Gloria-Soria A, Caccone A, Evans B, Schama R, Martins AJ, et al. Tracking the return of Aedes aegypti to Brazil, the major vector of the dengue, chikungunya and Zika viruses. PLoS Negl Trop Dis. 2017;11 (7):e0005653. , ¹⁰³103. Mousson L, Dauga C, Garrigues T, Schaffner F, Vazeille M, Failloux AB. Phylogeography of Aedes ( Stegomyia ) aegypti (L.) and Aedes ( Stegomyia ) albopictus (Skuse) (Diptera: Culicidae) based on mitochondrial DNA variations. Genet Res. 2005;86(1):1-11. , ¹²⁸128. Guzmán MG, Kourí G. Dengue: an update. Lancet Infect Dis. 2002;2(1):33-42. ]. Another reason could be the insufficiency of vaccination coverage, which should have favored the extension of the disease beyond its natural limits, particularly in the regions of Brazil where vaccination was not recommended, e.g., in northeast and southern Brazil [ ⁹⁰90. Vasconcelos PF, Rodrigues SG, Degallier N, Moraes MA, da Rosa JF, da Rosa ES, et al. An epidemic of sylvatic yellow fever in the southeast region of Maranhao state, Brazil, 1993-1994: epidemiologic and entomologic findings. Am J Trop Med Hyg. 1997;57(2):132-7. , ¹²⁹129. Romano AP, Costa ZG, Ramos DG, Andrade MA, Jayme Vde S, Almeida MA, et al. Yellow fever outbreaks in unvaccinated populations, Brazil, 2008-2009. PLoS Negl Trop Dis. 2014;8(3):e2740. ]. Nevertheless, YF now seems well established in the form of a deeply rooted jungle cycle, as shown by the numerous epizootics reported in recent years ( Fig. 6 ). Finally, the sudden population growth and unplanned urbanization that results in substandard housing, and inadequate water supply and waste management systems, at least partially explain the failure of preventive measures and the delay in the management of cases [ ⁸⁵85. Vasconcelos PFC, Bryant JE, da Rosa APAT, Tesh RB, Rodrigues SG, Barrett ADT. Genetic divergence and dispersal of yellow fever virus, Brazil. Emerg Infect Dis. 2004;10(9):1578-84. , ¹²⁸128. Guzmán MG, Kourí G. Dengue: an update. Lancet Infect Dis. 2002;2(1):33-42. ]. The vectorial competence of A. aegypti and A. albopictus reinforce the risk of YF extension in cities, especially in the overcrowded suburbs of major Brazilian cities [ ³3. Mondet B, Travassos da Rosa APA, Vasconcelos PFC. Les risques d'épidémisation urbaine de la fièvre jaune au Brésil par les vecteurs de la dengue: Aedes aegypti et Aedes albopictus. Bull Soc Pathol Exot. 1996;89(2):107-13. , ⁸⁴84. Couto-Lima D, Madec Y, Bersot MI, Campos SS, Motta MA, Santos FBD, et al. Potential risk of re-emergence of urban transmission of yellow fever virus in Brazil facilitated by competent Aedes populations. Sci Rep. 2017;7(1):4848. ].

The attempt to eliminate the YF during the twenty-first century, despite a relative failure, probably contained the risk of urban and peri-urban epidemics. For more than 50 years, Brazilian YF epidemics - and the most recent one was no exception - were sylvatic and involved wild vectors (Haemagogus and Sabethes , as well as non-anthropophilic Aedes , i.e. other species than A. aegypti and A. albopictus) and spared densely populated areas. So far, humans have been infected outside cities and their suburbs from multiple sylvatic foci [ ⁷³73. Moreira-Soto A, Torres MC, Lima de Mendonça MC, Mares-Guia MA, Dos Santos Rodrigues CD, Fabri AA, et al. Evidence for multiple sylvatic transmission cycles during the 2016-2017 yellow fever virus outbreak, Brazil. Clin Microbiol Infect. 2018; ]. However, the sylvatic cycle is expanding, and getting closer to the cities, infesting forest areas that could even be included in the conurbations of southern Brazil, notably in the states of Rio de Janeiro, São Paulo and Rio Grande do Sul, highlighting the risk of metropolitan epidemics. [ ⁸⁰80. Cardoso JC, de Almeida MA, dos Santos E, da Fonseca DF, Sallum MA, Noll CA, et al. Yellow fever virus in Haemagogus leucocelaenus and Aedes serratus mosquitoes, southern Brazil, 2008. Emerg Infect Dis. 2010;16(12):1918-24. – ⁸⁴84. Couto-Lima D, Madec Y, Bersot MI, Campos SS, Motta MA, Santos FBD, et al. Potential risk of re-emergence of urban transmission of yellow fever virus in Brazil facilitated by competent Aedes populations. Sci Rep. 2017;7(1):4848. , ¹³⁰130. Camargo-Neves VLF, Poletto DW, Rodas LAC, Pachioli ML, Cardoso RP, Scandar SAS, et al. Entomological investigation of a sylvatic yellow fever area in São Paulo state, Brazil. Cad Saude Publica. 2005;21(4):1278-86. , ¹³¹131. Cavalcante KRLJ, Tauil PL. Epidemiological characteristics of yellow fever in Brazil, 2000-2012. Epidemiol Serv Saude. 2016;25(1):11-20. ]. The epidemiological surveillance should be performed at two levels. On the one hand, the sentinel role of the monkeys that are the first to express the reemergence of the YF, dying from the disease, must be favored [ ⁷⁶76. Fernandes NCCA, Cunha MS, Guerra JM, Réssio RA, Cirqueira CDS, Iglezias SD, et al. Outbreak of yellow fever among nonhuman primates, Espirito Santo, Brazil, 2017. Emerg Infect Dis. 2017;23(12):2038-41. ]. On the other hand, the clinical diagnosis of YF index cases, which may reveal an increased risk of epidemic, must be reinforced. The “syndromic surveillance” approach recommended by US Centers for Disease Control and Prevention increases the sensitivity - and specificity - of first-line clinical detection [ ¹³²132. Fortaleza CMCB, Rocha R, Aragão VDN, Almeida RAMB. “Syndromic surveillance” and the reemergence of yellow fever in São Paulo state, Brazil, 2009. J Venom Anim Toxins incl Trop Dis. 2009;15(2):186-9. http://www.scielo.br/scielo.php?script=sci_arttext&pid=S1678-91992009000200002
http://www.scielo.br/scielo.php?script=s... ]. This method speeds up the diagnostic process, which is employed to organize case management and contain the epidemic.

The return of YF has led to a considerable increase in the genetic diversity of its South American genotype I, leading to the appearance of a new viral line [ ⁸⁹89. Mir D, Delatorre E, Bonaldo M, Lourenço-de-Oliveira R, Vicente AC, Bello G. Phylodynamics of yellow fever virus in the Americas: new insights into the origin of the 2017 Brazilian outbreak. Sci Rep. 2017; 7(1):7385. ]. The reasons for this diversification and its consequences, particularly as to transmissibility and virulence, remain to be clarified. One of the pending issues is the need to assess the capacity of the YF virus currently present in Brazil to invade peri-urban and urban environments spread by the A. aegypti and A. albopictus populations that abound [ ³3. Mondet B, Travassos da Rosa APA, Vasconcelos PFC. Les risques d'épidémisation urbaine de la fièvre jaune au Brésil par les vecteurs de la dengue: Aedes aegypti et Aedes albopictus. Bull Soc Pathol Exot. 1996;89(2):107-13. , ⁴4. Mondet B. Epidémiologie de la fièvre jaune au Brésil. Bull Soc Pathol Exot. 2001;94(3):260-7. ].

Two strategies - certainly not exclusive - enable the containment of YF: vector control and immunization of populations at risk. The former is very effective but expensive. It requires a constant effort wherever the risk of vector development is high. The recent epidemics of dengue, chikungunya and Zika in Brazil demonstrated the limits of this strategy [ ¹³³133. Penna MLF. Um desafio para a saúde pública brasileira: o controle do dengue. Cad Saude Publica. 2003;19(1):305-9. ]. However, integrated control - taking into account sanitation - and mutualized with other vector-borne diseases, is cost-effective and should be favored [ ¹³⁴134. Lima EP, Goulart MOF, Rolim Neto ML. Meta-analysis of studies on chemical, physical and biological agents in the control of Aedes aegypti. BMC Public Health. 2015;15:858. , ¹³⁵135. Fitzpatrick C, Haines A, Bangert M, Farlow A, Hemingway J, Velayudhan R. An economic evaluation of vector control in the age of a dengue vaccine. PLoS Negl Trop Dis. 2017;11(8):e0005785. ]. Vaccination against YF is based on a selective strategy - routine mandatory vaccinations in endemic areas of Brazil, voluntary vaccinations elsewhere such as the east and south of the country, and large-scale vaccinations of populations threatened by an epidemic. In Brazil, vaccine coverage is irregular, with a drop in coverage between 1990 and 2010, and insufficient in States where it is not compulsory [ ¹³⁶136. Shearer FM, Moyes CL, Pigott DM, Brady OJ, Marinho F, Deshpande A, et al. Global yellow fever vaccination coverage from 1970 to 2016: an adjusted retrospective analysis. Lancet Infect Dis. 2017;17(11):1209-17. ], which requires making a considerable effort to catch up on vaccinations in the event of an epidemic. This defective coverage results from recurrent vaccine shortages and poor tolerance [ ¹³⁷137. Martins Rde M, Pavão AL, de Oliveira PM, dos Santos PR, Carvalho SM, Mohrdieck R, et al. Adverse events following yellow fever immunization: report and analysis of 67 neurological cases in Brazil. Vaccine. 2014;32(49):6676-82. – ¹³⁹139. Barrett AD, Monath TP, Barban V, Niedrig M, Teuwen DE. 17D yellow fever vaccines: new insights. A report of a workshop held during the world congress on medicine and health in the tropics, Marseille, France, Monday 12 September 2005. Vaccine. 2007;25(15):2758-65. ].

Once the causative agent of the YF was identified in 1927 [ ⁴⁸48. Stokes A, Bauer JH, Hudson NP. Experimental transmission of yellow fever to laboratory animals. Am J Trop Med. 1928;8:103-64. ], the vaccine was discovered 10 years later [ ⁴⁹49. Theiler M, Smith HH. The use of yellow fever modified by in vitro cultivation for human immunization. J Exp Med. 1937;65:787-800. ]. It is a live virus attenuated by repeated passages into chicken embryos (YF 17D), and genetically stable. It replicates in the vaccinated individuals and confers protection for life [ ³⁴34. Monath T, Cetron MS, Teuwen DE. Yellow fever vaccine. In: Plotkin SA, Orenstein WA, Offit PA, editors. Vaccines. 5th ed. Philadelphia: Saunders Elsevier; 2008. p. 959-1055. , ¹³⁸138. Monath TP, Woodall JP, Gubler DJ, Yuill TM, Mackenzie JS, Martins RM, et al. Yellow fever vaccine supply: a possible solution. Lancet. 2016;387(10028):1599-600. , ¹³⁹139. Barrett AD, Monath TP, Barban V, Niedrig M, Teuwen DE. 17D yellow fever vaccines: new insights. A report of a workshop held during the world congress on medicine and health in the tropics, Marseille, France, Monday 12 September 2005. Vaccine. 2007;25(15):2758-65. ]. The effectiveness of the vaccine in controlling YF has been emphasized above in relation to its epidemiological description of the in both Africa and the Americas. In the current Brazilian context, vaccination of at-risk populations, including those living outside endemic areas, appears to be a strategy of choice provided that at least 80% of the resident population is covered to obtain an effective herd immunity [ ¹³⁹139. Barrett AD, Monath TP, Barban V, Niedrig M, Teuwen DE. 17D yellow fever vaccines: new insights. A report of a workshop held during the world congress on medicine and health in the tropics, Marseille, France, Monday 12 September 2005. Vaccine. 2007;25(15):2758-65. ]. However, global production - about 80 million doses annually - is insufficient in some years to cover the needs, i.e. routine newborn vaccination, immunization of travelers and protection of populations at risk of epidemic [ ⁵⁴54. Barrett ADT. Yellow fever live attenuated vaccine: a very successful live attenuated vaccine but still we have problems controlling the disease. Vaccine. 2017;35(44):5951-5. , ¹³⁸138. Monath TP, Woodall JP, Gubler DJ, Yuill TM, Mackenzie JS, Martins RM, et al. Yellow fever vaccine supply: a possible solution. Lancet. 2016;387(10028):1599-600. ]. The reduction of the vaccine dose administered - up to one-fifth of the recommended dose - conferred sufficient immunity and would allow, in the event of an epidemic, to respond to the needs, although these results require confirmation in real-life situations [ ⁵⁴54. Barrett ADT. Yellow fever live attenuated vaccine: a very successful live attenuated vaccine but still we have problems controlling the disease. Vaccine. 2017;35(44):5951-5. , ¹³⁹139. Barrett AD, Monath TP, Barban V, Niedrig M, Teuwen DE. 17D yellow fever vaccines: new insights. A report of a workshop held during the world congress on medicine and health in the tropics, Marseille, France, Monday 12 September 2005. Vaccine. 2007;25(15):2758-65. – ¹⁴²142. Visser LG, Roukens AH. Modelling a way out of yellow fever. Lancet. 2016; 388(10062):2847-8. ].

Another important issue is the incidence of serious adverse events (SAE). In addition to vaccine hypersensitivity and anaphylactic shock, SAEs were categorized into two groups: YFV-associated neurotropic disease (YFV-AND), including encephalitis, myelitis, acute disseminated encephalo-myelitis, and Guillain-Barré syndrome, and YF-vaccine-associated viscerotropic disease (YDV-AVD) responsible for multi-organ failure [ ¹³⁹139. Barrett AD, Monath TP, Barban V, Niedrig M, Teuwen DE. 17D yellow fever vaccines: new insights. A report of a workshop held during the world congress on medicine and health in the tropics, Marseille, France, Monday 12 September 2005. Vaccine. 2007;25(15):2758-65. ]. Risk factors are age (young children under 6 months and adults over 50), pregnancy and immunodeficiency. Most SAEs concern primary vaccination [ ¹⁴³143. Thomas RE, Lorenzetti DL, Spragins W, Jackson D, Williamson T. The safety of yellow fever vaccine 17D or 17DD in children, pregnant women, HIV+ individuals, and older persons: systematic review. Am J Trop Med Hyg. 2012;86(2):359-72. , ¹⁴⁴144. Seligman SJ, Cohen JE, Itan Y, Casanova JL, Pezzullo JC. Defining risk groups to yellow fever vaccine-associated viscerotropic disease in the absence of denominator data. Am J Trop Med Hyg. 2014;90(2):267-71. ]. Based on meta-analyses in many countries with reliable pharmacovigilance, the incidence of SAEs was estimated to be 11.1-15.6 per million vaccinated persons, including 6.6 YFV-AND and YFV-AVD cumulated, with wide variations depending on the country [ ¹⁴⁵145. Thomas RE, Lorenzetti DL, Spragins W, Jackson D, Williamson T. Active and passive surveillance of yellow fever vaccine 17D or 17DD-associated serious adverse events: systematic review. Vaccine. 2011;29(28):4544-55. ]. These are linked both to the surveillance system and to the recruitment of vaccinated persons: in YF-free regions, the latter are most often travelers whose age is on average significantly higher than people from endemic countries where routine immunization targets young children. Despite the high incidence of SAEs, the risk-benefit profile remains extremely favorable for vaccination in endemic areas [ ¹³⁹139. Barrett AD, Monath TP, Barban V, Niedrig M, Teuwen DE. 17D yellow fever vaccines: new insights. A report of a workshop held during the world congress on medicine and health in the tropics, Marseille, France, Monday 12 September 2005. Vaccine. 2007;25(15):2758-65. ]. The mortality due to SAEs is below one per million vaccinated people [ ¹⁴⁵145. Thomas RE, Lorenzetti DL, Spragins W, Jackson D, Williamson T. Active and passive surveillance of yellow fever vaccine 17D or 17DD-associated serious adverse events: systematic review. Vaccine. 2011;29(28):4544-55. ], which must be compared with the 33% case fatality rate of YF in Brazil ( Table 1 ). In addition, it is likely that the risk of SAEs increases during large-scale vaccination campaigns due to reduced attention to risk factors in vaccinated people and conditions of storage and vaccine administration. The vaccinations carried out in Brazil and Argentina during the recent YF outbreak confirmed these data, showing an SAEs incidence ranging from 8.3 to 12.4 per million respectively, mainly involving people at risk, especially those over 50 years old [ ¹³⁷137. Martins Rde M, Pavão AL, de Oliveira PM, dos Santos PR, Carvalho SM, Mohrdieck R, et al. Adverse events following yellow fever immunization: report and analysis of 67 neurological cases in Brazil. Vaccine. 2014;32(49):6676-82. , ¹⁴⁶146. Biscayart C, Carrega ME, Sagradini S, Gentile A, Stecher D, Orduna T, et al. Yellow fever vaccine-associated adverse events following extensive immunization in Argentina. Vaccine. 2014;32(11):1266-72. ]. Considering the risks of urban epidemics and incidence of SAEs, it is urgent to develop a more tolerable vaccine. The vaccine strategy will need to be reconsidered to extend vaccine coverage to the whole country, including major urban metropolises.

Conclusion

The physiognomy of YF has reemerged abruptly over the last 50 years while the disease was likely to be controlled. Consequently, it is no longer a question of its eradication, if only because of the sylvatic foci present on two continents, but rather of limiting the epidemic risk [ ¹⁴⁷147. WHO. Eliminate yellow fever epidemics (EYE): a global strategy, 2017-2026. Wkly Epidemiol Rec. 2017;92(16):193-204. ].

The reservoir of YF, both in Africa and the Americas, is the mosquito, especially the sylvatic species that maintain the jungle cycle. The short viremia and definitive immunity - or death - that follow the viral infection in mammals do not allow their consideration as a proper virus reservoir.

However, they ensure amplification of the latter and, in the Americas in particular, are an alarm signal of viral reemergence that can result in human outbreaks able to extend into urban areas.

The history of YF, especially its installation in the Americas five centuries ago, taught us that the virus and its vector presented a remarkable capacity for environmental adaptation. The pair seem to react very quickly to the conditions that they face. While until 1960, the virus was spread by boat - limited to transport through mosquitos - which required time and allowed the implementation of preventive or remedial measures, it is now rapidly spread via aircraft carrying infected humans, a scenario that is more difficult to control.

However, there are flaws in the transmission of the YF, as evidenced by its absence from Asia. The emergence or re-emergence of vector-borne diseases depends on complex, entangled biological, climatic, ecological, socio-economic and political factors [ ¹⁴⁸148. Reiter P. Global warming and mosquito-borne disease in USA. Lancet. 1996; 348(9027):622. ]. Three conditions are necessary to produce YF epidemics: a) the introduction of the virus into a non-immune human community, b) presence of competent and anthropophilic vectors and, c) insufficiency of prevention and/or adequate management. On the other hand, there are two weapons available to fight YF: vector control and immunization of human populations [ ¹⁴⁷147. WHO. Eliminate yellow fever epidemics (EYE): a global strategy, 2017-2026. Wkly Epidemiol Rec. 2017;92(16):193-204. ]. The first has the advantage of allowing the control of many other parasitic and viral diseases transmitted by arthropods, and may result in the mutualization of resources. It involves financial and ecological constraints that can limit its application and effectiveness. Immunization is both cheaper and very effective, subject to strict and permanent application.

The objectives of the WHO are therefore to protect the at-risk population, prevent international spread and rapidly contain epidemics. These objectives include a prevention component through appropriate urban development and an immediate response in the event of an YF outbreak by combining vector control against Aedes larvae and adults, and preventive mass immunization [ ¹⁴⁹149. WHO. Yellow Fever - Brazil. Disease outbreak new, 9 March 2018: http://www.who.int/csr/don/09-march-2018-yellow-fever-brazil/en/ (accessed 17 Apr 2018).
http://www.who.int/csr/don/09-march-2018... ]. In Brazil, preventive vaccination is underway. However, it is necessary to reconsider the vaccination schedule. While waiting for a safer YF vaccine, vector control measures and epidemiological surveillance should be strengthened to initiate emergency large-scale vaccination campaigns along two lines: monkey mortality [ ⁷⁶76. Fernandes NCCA, Cunha MS, Guerra JM, Réssio RA, Cirqueira CDS, Iglezias SD, et al. Outbreak of yellow fever among nonhuman primates, Espirito Santo, Brazil, 2017. Emerg Infect Dis. 2017;23(12):2038-41. , ¹⁵⁰150. Almeida MAB, Cardoso JC, dos Santos E, da Fonseca DF, Cruz LL, Faraco FJC, et al. Surveillance for yellow fever virus in non-human primates in southern Brazil, 2001-2011: a tool for prioritizing human populations for vaccination. PLoS Negl Trop Dis. 2014;8(3):e2741. ] and syndromic surveillance in sentinel hospitals [ ¹³²132. Fortaleza CMCB, Rocha R, Aragão VDN, Almeida RAMB. “Syndromic surveillance” and the reemergence of yellow fever in São Paulo state, Brazil, 2009. J Venom Anim Toxins incl Trop Dis. 2009;15(2):186-9. http://www.scielo.br/scielo.php?script=sci_arttext&pid=S1678-91992009000200002
http://www.scielo.br/scielo.php?script=s... ].

Public health strategies must combine both scientific and political criteria. The history of YF stressed, as many authors have already noted, that the opinions of scientists - sometimes giving rise to expertise followed by the authorities - often came from assertions based on subjective arguments rather than evidence based on observations validated experimentally. Controversies conceal ideological cleavages, even political ones, which divert the public debate from its objectives of prevention and management, make them lose their effectiveness, and involve useless and considerable expenses [ ¹⁵15. Lódola S, Góis Jr E. Theories about the propagation of yellow fever: the scientific debate in the São Paulo press between 1895 and 1903. Hist Cienc Saude Manguinhos 2015;22(3):687-704. http://www.scielo.br/hcsm (accessed 18 Apr 2018).
http://www.scielo.br/hcsm... , ¹⁶16. Ackerknecht EH. Anticontagionism between 1821 and 1867. Int J Epidemiol. 2009;38(1):7-21. ].

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