Clinical and parasitological impact of short-term treatment using miltefosine and allopurinol monotherapy or combination therapy in canine visceral leishmaniasis

Ayres, Eveline da Cruz Boa Sorte; Dias, Álvaro Felipe de Lima Ruy; Monteiro, Bruna Ribeiro Gomes; Pazzini, Sarah Szimanski; Barbosa, Mateus Elias Chagas; Silva, Eveliny Barroso da; Macedo, Luis Felipe da Cruz; Sousa, Valéria Régia Franco; Dutra, Valéria; Nakazato, Luciano; Almeida, Arleana do Bom Parto Ferreira de

doi:10.1590/S1984-29612022040

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Revista Brasileira de Parasitologia Veterinária

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Original Article • Rev. Bras. Parasitol. Vet. 31 (3) • 2022 • https://doi.org/10.1590/S1984-29612022040 copy

Clinical and parasitological impact of short-term treatment using miltefosine and allopurinol monotherapy or combination therapy in canine visceral leishmaniasis

Impacto clínico e parasitológico do tratamento de curta duração com miltefosina e alopurinol em monoterapia ou terapia combinada na leishmaniose visceral canina

Authorship SCIMAGO INSTITUTIONS RANKINGS

Abstract

Canine visceral leishmaniasis is an endemic zoonosis in Brazil. Dogs are the main hosts in urban environments. The treatment has gained popularity since the Brazilian government authorized miltefosine for canine treatment. The aim of this study was to investigate the clinical and parasitological impact of short-term treatment with miltefosine and allopurinol, alone and in combination. We evaluated the ability of pharmacotherapy to reduce clinical signs of disease, antibody levels using the indirect fluorescence antibody test (IFAT) and skin parasite load via qPCR after 28 days of treatment. The therapeutic protocols promoted a significant decline in clinical signs and in the skin parasite load in dogs (p < 0.01). We observed a moderate correlation between the skin parasite load and the clinical score in all three treatment groups (r > 0.5) Antibody levels did not decrease in this short period. It was concluded that the treatment with allopurinol reduced the number of parasites in the skin of dogs with visceral leishmaniasis in the short term. However, its efficiency is potentiated when associated with miltefosine.

Keywords:
Miltefosine; Allopurinol; Leishmania infantum; qPCR; skin

Clinical Signs	Miltefosine		Allopurinol		Miltefosine + Allopurinol
Clinical Signs	D0 (n / %)	D29 (n / %)	D0 (n / %)	D29 (n / %)	D0 (n / %)	D29 (n / %)
Anorexia	13 / 86.7	8 / 53.3	11 / 73.3	3 / 20	10 / 66.7	5 / 33.3
Apathy	11 / 73.3	4 / 27	7 / 46.7	2 / 13.3	11 /73.3	2 / 13.3
Weigh loss	10 / 66.7	6 / 40	11 / 73.3	6 / 40	8 / 53.3	5 / 33.3
Lymph adenomegaly	12 / 80	10 / 66.7	11 / 73.3	6 / 40	13 / 86.7	10 / 66.7
Muscle atrophy	4 / 27	2 / 13.3	3 / 20	1 / 6.7	1 / 6.7	11 / 6.7
Arthropathy	3 / 20	1 / 6.7	7 / 46.7	3 / 20	6 / 40	5 / 33.3
Digestive Disorders	3 / 20	3 / 20	1 / 6.7	0 / 0	3 / 20	0 / 0
Splenomegaly	1 / 6.7	0 / 0	5 / 33.3	3 / 20	6 / 40	2 / 13.3
Polyuria/polydipsia	3 / 20	3 / 20	5 / 33.3	3 / 20	3 / 20	1 / 6.7
Epistaxis	3 / 20	1 / 6.7	2 / 13.3	0 / 0	1 / 6.7	0 / 0
Pale mucous membranes	5 / 33.3	5 / 33.3	6 / 40	3 / 20	7 / 46.7	2 / 13.3
Dermatological changes	14 / 93.4	13 / 86.7	15 / 100	13 / 86.7	14 / 93.4	14 / 93.4
Ophthalmic changes	8 / 53.3	7 / 46.7	5 / 33.3	4 / 27	12 / 80	7 / 46.7

	Miltefosine (n = 15)
	D0	D29	P-value
Clinical Signs	12.5 ± 6.0	7.8 ± 5,5	< 0.01
IFAT	376.0 ± 267.8	405.0 ± 246.5	0.76
	Allopurinol (n = 15)
	D0	D29	P-value
Clinical Signs	14.2 ± 8.4	5.7 ± 5.3	< 0.01
IFAT	285.3 ± 203.3	381.3 ± 209.9	0.99
	Miltefosine + Allopurinol (n = 15)
	D0	D29	P-value
Clinical Signs	14.5 ± 7.4	6.8 ± 4.8	< 0.01
IFAT	354.6 ± 257.8	429.3 ± 191.5	0.82

Miltefosine (n = 15)
D0	D29	P-value
4.5x10⁷ ± 1.5x10⁸	4.6x10⁶ ± 1.2x10⁷	0.05
Allopurinol (n = 15)
D0	D29	P-value
1.2x10⁷ ± 2.3x10⁷	1.1x10⁶ ± 2.8x10⁶	< 0.01
Miltefosine + Allopurinol (n = 15)
D0	D29	P-value
1.2x10⁷ ± 1.9x10⁷	1.0x10⁶ ± 1.3x10⁶	< 0.01

	qPCR X Clinical Signs	qPCR X IFAT
	(r)	(r)
Miltefosine	0.60	0.17
Allopurinol	0.55	0.00
Milefosine + Allopurinol	0.60	0.04

Colégio Brasileiro de Parasitologia Veterinária FCAV/UNESP - Departamento de Patologia Veterinária, Via de acesso Prof. Paulo Donato Castellane s/n, Zona Rural, , 14884-900 Jaboticabal - SP, Brasil, Fone: (16) 3209-7100 RAMAL 7934 - Jaboticabal - SP - Brazil
E-mail: cbpv_rbpv.fcav@unesp.br

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[1] *Corresponding author: Arleana do Bom Parto Ferreira de Almeida. E-mail:arleferreira@gmail.com