Role of VPAC1 and VPAC2 receptors in the etiology of pregnancy rhinitis: an experimental study in rats

Ulkumen, Burak; Batir, Muhammet Burak; Ulkumen, Burcu Artunc; Pala, Halil Gursoy; Vatansever, Seda; Cam, Sirri

doi:10.1016/j.bjorl.2020.06.015

Abstract

Introduction:

Pregnancy rhinitis is a common sex hormone-related otorhinolaryngological disorder. There are some epidemiological and physiological studies on pregnancy rhinitis, but histopathological and biomolecular changes have not been studied thoroughly.

Objectives:

The receptors VPAC1 and VPAC2 are known for their roles in allergic rhinitis. On the other hand, activation of subclinical allergy has been suggested in the pathophysiology of pregnancy rhinitis. Therefore, we aimed to compare the physiological and gestational pattern of VPAC1 and VPAC2 expression in rat nasal mucosa.

Methods:

Twenty adult Wister albino female rats were enrolled into the study. Two groups constituted as 10 control (group A) and 10 pregnant (group B) rats. They were fed ad libitum and sheltered at room temperature (22°±2°C). The rats were sacrificed at the 20th day of gestation by intraperitoneal injection of 400mg/kg Na-pentobarbitone. Then, 10 – 15 mL of blood was taken, and samples were reserved for the detection of serum estradiol and progesterone levels by ELISA test. The nasal septum was resected and divided in half for immunohistochemical analyses and real time polymerase chain reaction testing of VPAC1 and VPAC2.

Results:

VPAC1 and VPAC2 were found to be in all layers of septal specimens, but the immunostaining of surface epithelium was more distinct in specimens of both groups. We demonstrated higher overall staining intensity in the pregnant group. PCR revealed significant increase in expression of VPAC1 (p = 0.023) and VPAC2 (p = 0.021) in pregnant group when compared with control group. In addition, we demonstrated upregulatory effect of estradiol and progesterone on the vasoactive intestinal peptide receptor expression.

Conclusions:

Gestational up-regulation of nasal VPAC1 and VPAC2 was shown both by PCR and immunohistochemical analysis. These findings support the hypothesis that PR is caused by the activation of subclinical allergy that is present before pregnancy.

Keywords
Pregnancy rhinitis; VPAC1; VPAC2; Estradiol; Progesterone

Resumo

Introdução:

A rinite gestacional é um distúrbio comum da otorrinolaringologia relacionado a hormônios sexuais. Existem alguns estudos epidemiológicos e fisiológicos sobre rinite gestacional, mas as alterações histopatológicas e biomoleculares ainda não foram estudadas completamente.

Objetivo:

Os receptores VPAC1 e VPAC2 são conhecidos por seu papel na rinite alérgica. Por outro lado, a ativação da alergia subclínica tem sido sugerida na fisiopatologia da rinite gestacional. Portanto, objetivamos comparar o padrão fisiológico e gestacional da expressão de VPAC1 e VPAC2 na mucosa nasal de ratos.

Método:

Vinte ratas fêmeas Wistar albinas adultas foram incluídas no estudo. Os dois grupos foram divididos em 10 ratas; controle (grupo A) e 10 ratas prenhes (grupo B). Elas foram alimentadas ad libitum e abrigadas em temperatura ambiente (22° ±2° C). Sacrificamos as ratas no 20° dia de gestação por injeção intraperitoneal de 400 mg/kg de sódio-pentobarbital. Em seguida, foram coletados 10 a 15 mL de sangue e as amostras foram reservadas para a detecção dos níveis séricos de estradiol e progesterona pelo método Elisa. O septo nasal foi ressecado e dividido em 2 para análises imuno-histoquímicas e testes de reação em cadeia da polimerase em tempo real, RT-PCR, de VPAC1 e VPAC2.

Resultados:

VPAC1 e VPAC2 foram encontrados em todas as camadas da amostra septal, mas a imunocoloração do epitélio de superfície foi mais distinta nas amostras de ambos os grupos. Demonstramos maior intensidade geral de coloração no grupo gestante. A reação de polimerase em cadeia revelou aumento significante na expressão de VPAC1 (p = 0,023) e VPAC2 (p = 0,021) no grupo gestante quando comparado ao grupo controle. Além disso, demonstramos um efeito up-regulador do estradiol e progesterona na expressão do receptor peptídeo intestinal vasoativo.

Conclusão:

A up-regulação gestacional dos receptores VPAC1 e VPAC2 nasais foi demonstrada tanto por reação de polimerase em cadeia quanto por análise imuno-histoquímica. Esses achados corroboram a hipótese de que a rinite gestacional é causada pela ativação de alergia subclínica presente antes da gestação.

PALAVRAS-CHAVE
Rinite gestacional; VPAC1; VPAC2; Estradiol; Progesterona

Introduction

Fluctuations in serum gonadocorticoid levels cause some adverse Otorhinolaryngological (ORL) signs and symptoms.¹1 D’haeseleer E, Depypere H, Claeys S, Van Borsel J, Van Lierde K. The menopause and the female larynx, clinical aspects, and therapeutic options: a literature review. Maturitas. 2009;64:27-32.,²2 Turan M, Ucler R, Garca MF, Kurdoglu Z, Cankaya H, Ayral A, et al. The Relationship Between Hearing Thresholds and Hyperandrogenism in Polycystic Ovary Syndrome. Med Sci Monit. 2016;22:4380-5. It is known that physiological, pathological or iatrogenic conditions cause change in gonadocorticoid levels.³3 Kumar R, Hayhurst KL, Robson AK. Ear, nose, and throat manifestations during pregnancy. Otolaryngol Head Neck Surg. 2011;145:188-98.,⁴4 Shoffel-Havakuk H, Carmel-Neiderman NN, Halperin D, Shapira Galitz Y Levin D, Haimovich Y, et al. Menstrual Cycle, Vocal Performance, and Laryngeal Vascular Appearance: An Observational Study on 17 Subjects. J Voice. 2018;32:226-33.,⁵5 Kabil Kucur S, Seven A, Yuksel B, Kucur C, Sencan H, Gozukara I, et al. Alterations in nasal mucociliary activity in polycystic ovary syndrome. Eur J Obstet Gynecol Reprod Biol. 2016;207:169-72. Pregnancy, as a physiological condition, also induces some sex hormone- related ORL symptoms.⁶6 Bhagat DR, Chowdhary A, Verma S, Jyotsana. Physiological changes in ENT during pregnancy. Indian J Otolaryngol Head Neck Surg. 2006;58:268-70.,⁷7 Shiny Sherlie V, Varghese A. ENT Changes of Pregnancy, and Its Management. Indian J Otolaryngol Head Neck Surg. 2014;66:6-9. One of them is Pregnancy Rhinitis (PR), which is defined as the presence of nasal congestion, rhinorrhea and sneezing which arise particularly during gestation and subside in 3 weeks’ time after delivery. In addition, history of allergy and other nasal pathologies are defined as exclusion criteria for PR.³3 Kumar R, Hayhurst KL, Robson AK. Ear, nose, and throat manifestations during pregnancy. Otolaryngol Head Neck Surg. 2011;145:188-98.,⁸8 Ulkumen B, Ulkumen BA, Pala HG, Celik O, Sahin N, Karaca G, et al. Pregnancy rhinitis in Turkish women: Do gestational week, BMI and parity affect nasal congestion? Pak J Med Sci. 2016;32:950-4.

PR leads to a predisposition to snoring and even obstructive sleep apnea syndrome, which induces some maternal and fetal morbidities.⁹9 Ayrim A, Keskin E, Ozol D, Onaran Y Yidirim Z, Kafali H. Influence of self-reported snoring and witnessed sleep apnea on gestational hypertension and fetal outcome in pregnancy. Arch Gynecol Obstet. 2011;283:195-9.,¹⁰10 Franklin K, Holmgren PA, Jonssen F. Snoring, pregnancy-induced hypertension, and growth retardation of the fetus. Chest. 2000;117:137-41.,¹¹11 Somoskovi A, Bartfai Z, Tamasi L, Kocsis J, Puho E, Czeizel A. Population-based case-control study of allergic rhinitis during pregnancy for birth outcomes. Eur J Obstet Gynecol Reprod Biol. 2007;131:21-7. The pathophysiology of PR is still not fully understood. But increased serum levels of particular hormones (Progesterone [PG], Estradiole [E2], placental growth hormone, human chorionic gonadotropin) have been asserted as the triggering factor.¹⁰10 Franklin K, Holmgren PA, Jonssen F. Snoring, pregnancy-induced hypertension, and growth retardation of the fetus. Chest. 2000;117:137-41. Activation of subclinical allergy has also been suggested as the pathophysiology of PR by some studies.³3 Kumar R, Hayhurst KL, Robson AK. Ear, nose, and throat manifestations during pregnancy. Otolaryngol Head Neck Surg. 2011;145:188-98.,¹²12 Ellegård EK. Special considerations in the treatment of pregnancy rhinitis. Womens Health (Lond). 2005;1:105-14.,¹³13 Toppozada H, Michaels L, Toppozada M, El-Ghazzawi I, Talaat M, Elwany S. The human respiratory nasal mucosa in pregnancy. An electron microscopic and histochemical study. J Laryngol Otol. 1982;96:613-26.,¹⁴14 Ellegård E, Karlsson G. IgE-mediated reactions and hyperreactivity in pregnancy rhinitis. Arch Otolaryngol Head Neck Surg. 1999;125:1121-5. However, there is no high level of evidence to support that Allergic Rhinitis (AR) and PR share similar pathophysiological processes. In addition, the impact of sex hormones on nasal mucosa has been studied in various aspects.¹⁵15 Toppozada H. The human nasal mucosa in the menopause (a histochemical and electron microscopic study). J Laryngol Otol. 1988;102:314-8.,¹⁶16 Toppozada H, Toppozada M, El-Ghazzawi I, Elwany S. The human respiratory nasal mucosa in females using contraceptive pills. An ultramicroscopic and histochemical study. J Laryngol Otol. 1984;98:43-51.,¹⁷17 Philpott CM, Wild DC, Wolstensholme CR, Murty GE. The presence of ovarian hormone receptors in the nasal mucosa and their relationship to nasal symptoms. Rhinology. 2008;46:221-5.,¹⁸18 Horie S, Yamaki A, Takami S. Presence of Sex Steroid-Metabolizing Enzymes in the Olfactory Mucosa of Rats. Anat Rec (Hoboken). 2017;300:402-14.,¹⁹19 Karaer I, Tuncay G. The effect of premature ovarian insufficiency on nasal mucociliary clearance time. Gynecol Endocrinol. 2019;25:1-4.,²⁰20 Konno A, Terada N, Okamoto Y Effects of female hormones on the muscarinic and alpha 1-adrenergic receptors of the nasal mucosa. An experimental study in guinea pigs. ORL J Otorhinolaryngol Relat Spec. 1986;48:45-51. But there is very limited data regarding histopathological and biomolecular changes in the nasal mucosa of patients having PR.²¹21 Orban N, Maughan E, Bleach N. Pregnancy-induced rhinitis. Rhinology. 2013;51:111-9.,²²22 Verma AK, Manohar M, Upparahalli Venkateshaiah S, Mishra A. Neuroendocrine cells derived chemokine Vasoactive Intestinal Polypeptide (VIP) in allergic diseases. Cytokine Growth Factor Rev. 2017;38:37-48.

Vasoactive Intestinal Peptide (VIP) is a peptide hormone which is known to be secreted in various tissues.²³23 Abad C, Tan YV. Immunomodulatory Roles of PACAP and VIP: Lessons from Knockout Mice. J Mol Neurosci. 2018;66:102-13. VIP is mainly known for its immunomodulatory functions.²⁴24 Kim DH, Park IH, Cho JS, Lee YM, Choi H, Lee HM. Alterations of vasoactive intestinal polypeptide receptors in allergic rhinitis. Am J Rhinol Allergy. 2011;25:44-7. It takes part in regulation of immune response through 4 receptors (VPAC-1, VPAC-2, PAC1, CRTH2). In the upper respiratory tract, VIP mainly functions via VPAC1 and VPAC2. On the other hand, upregulation of nasal VPAC-1 and VPAC-2 expression was reported in AR.²⁵25 Voice JK, Dorsam G, Lee H, Kong Y Goetzl EJ. Allergic diathesis in transgenic mice with constitutive T-cell expression of inducible vasoactive intestinal peptide receptor. FASEB J. 2001;15:2489-96. The link between these two receptor proteins and allergy was also shown in some other studies.²⁴24 Kim DH, Park IH, Cho JS, Lee YM, Choi H, Lee HM. Alterations of vasoactive intestinal polypeptide receptors in allergic rhinitis. Am J Rhinol Allergy. 2011;25:44-7.,²⁶26 Samarasinghe AE, Hoselton SA, Schuh JM. The absence of VPAC2 leads to aberrant antibody production in Aspergillus fumigatus sensitized and challenged mice. Peptides. 2011;32:131-7. In consideration of these findings we hypothesize that the pattern of VPAC-1 and VPAC-2 expression would significantly change in the nasal mucosa of pregnant rats when compared with non-pregnant ones. Discovery of any gestational change in nasal expression of these 2 biomolecules may partly unveil the histopathological background of PR. Besides, we may have the opportunity to reveal a common pathway which would link up the physiopathology of AR and PR. By this means new treatment strategies could be proposed for PR.

As far as we know, the nasal expression of VPAC1 and VPAC2 has not been studied in relation to pregnancy before. In this study, we explored the physiological pattern of VPAC-1 and VPAC-2 expression in rat nasal mucosa as well as the impact of pregnancy on these receptors. Additionally, the effect of PG and E2 on the expression of these 2 receptors was also studied.

Methods

Animals

This animal experimental study was done in institutional experimental animals’ research and application center in accordance with the accepted policy on the use of animals. Institutional Animal Ethics Committee approved the overall procedures.

Twenty adults (8-12 week old) Wister albino female rats were involved in the study. The rats were fed ad libitum and sheltered at room temperature (22°±2°C) on a 12 h light-dark cycle. All procedures were done during daytime. Thirty-two female rats were housed together with male rats in the ratio of 4/1 for overnight. The following morning vaginal smears of female rats were examined for sperm existence. We accept the observation of sperm as the day 0 of the gestation as described before.²⁷27 Agematsu Y Ikadai H, Amao H. Early detection of pregnancy of the rat. Jikken Dobutsu. 1983;32:209-12.,²⁸28 Lohmiller JJ, Swing SP. Reproduction and Breeding. In: Suckow MA, Weisbroth SH, Franklin CL, editors. The laboratory rat. Boston BOS. Elsevier; 2006. p. 147-65.,²⁹29 Ulkumen B, Artunc Ulkumen B, Batir MB, Pala HG, Vatansever S, Cam S. Impact of Pregnancy and Glucocorticoid Treatment on NF-KB and MUC5AC in Mucosa of Rat Larynx. J Voice. 2021;35:342-8. The first 10 rats with negative and 10 rats with positive vaginal smear were chosen from among 32 rats as the control group (Group A) and the pregnant group (Group B), respectively. The remaining 12 rats were not enrolled into the study. Gestation period of Wister albino rat has been reported as approximately 22 (21 – 26) days.²⁹29 Ulkumen B, Artunc Ulkumen B, Batir MB, Pala HG, Vatansever S, Cam S. Impact of Pregnancy and Glucocorticoid Treatment on NF-KB and MUC5AC in Mucosa of Rat Larynx. J Voice. 2021;35:342-8. For this reason, we sacrificed the rats at 20thday of gestation by intraperitoneal injection of 400mg/kg Na-pentobarbiton.³⁰30 Alvites RD, Caseiro AR, Pedrosa SS, Branquinho ME, Varejão ASP, Maurício AC. The Nasal Cavity of the Rat and Mouse-Source of Mesenchymal Stem Cells for Treatment of Peripheral Nerve Injury. Anat Rec (Hoboken). 2018;301:1678-89. After the loss of consciousness and righting reflex, 10- 15mL of blood was taken by a 23G needle.. Blood samples were reserved for the detection of serum E2 and PG levels by ELISA.

We then shaved the nasal dorsum (Fig. 1a). We separated the nasal bones from the maxilla in an upward manner and revealed the nasal cavity macroscopically as described by Alvites et al. (Fig. 1b).³⁰30 Alvites RD, Caseiro AR, Pedrosa SS, Branquinho ME, Varejão ASP, Maurício AC. The Nasal Cavity of the Rat and Mouse-Source of Mesenchymal Stem Cells for Treatment of Peripheral Nerve Injury. Anat Rec (Hoboken). 2018;301:1678-89. We then resected the cartilaginous part of the septum, taking care not to damage the mucosal integrity. The resected specimen was divided in half for immunohistochemical analyses and real- time Polymerase Chain Reaction testing (PCR).

Figure 1
(a) External view of rat’s rhinarium (dorsal hair shaved), (b) Nasal roof (Os nazale) are mobilized in upward direction, (c) Internal macroscopic view of both nasal cavities (Cavum nasi) after removal of nasal roof. The septum (Septum nasi osseum), middle nasal chonca (Concha nasalis media) and frontal bone (Os frontale) are seen. Arrow: Os nazale; 1 and 2: Middle nasal conchae; 3: Septum with respiratory epithelium; 4: Vomer with olfactory mucosa; * Frontal bone.

Immunohistochemistry (IHC)

The pecimens were fixed by formaldehyde solution of 10% for 24h. Next, dehydration and paraffin emplacement were accomplished. Paraffin blocks were dissected at a 4μm thickness. For primary examination, Hematoxylin-Eosin (H&E) dye was utilized. “VPAC1 Antibody (B-4): sc-377152” and “VPAC2 Antibody (AS69): sc-52795” were used in accordance with the recommended protocols for immunohistochemical detection of VPAC1 and VPAC2 (Santa Cruz Biotechnology, Inc., TX, USA). Concentration of VPAC1 and VPAC2 was 200μg/mL and 50μg/mL, respectively. The control of immunospecifity of each group was performed by the replacement of primary antibodies with Phosphate Buffered Saline (PBS). Immunohistochemical pattern of VPAC1 and VPAC2 expression was examined by light microscopy (Olympus BX41). Immunostaining for VPAC1 and VPAC2 was evaluated in terms of structural layers of nasal mucosa.

ELISA

EDTA, sodium citrate and heparin were mixed with the blood samples. Then the mixture was centrifuged at 3000 rpm for 10min. The supernatant stored at −80°C. Rat E2 (estradiol) ELISA Kit and General Progesterone (PG) ELISA Kit were used for quantitative measurement of serum E2 and PG levels, respectively (MyBioSource, Inc., CA, USA).²⁹29 Ulkumen B, Artunc Ulkumen B, Batir MB, Pala HG, Vatansever S, Cam S. Impact of Pregnancy and Glucocorticoid Treatment on NF-KB and MUC5AC in Mucosa of Rat Larynx. J Voice. 2021;35:342-8.

RNA extraction and quantitative Real-Time PCR (qRT-PCR) analyses

Total RNA extraction was carried out from the laryngeal mucosa with using TRIzol® Reagent in the combination with the PureLink® RNA Mini Kit (Thermo Fisher Scientific, 12183555). RNA expression levels of VPCA1 and VPCA2 were acquired from the extracted RNA samples with using forward VPCA1F1 primer 5-ATCAACTCCTCCCTGTGGTG-3', reverse VPCA1R1 primer 5-GGGCTGCTATCATTCTTCCC-3', forward VPCA2F1 5-GGACAGTGTGCTCTACTCCA-3', reverse VPCA2R1 5-GCCAGTAGAAGTTCGCCATG-3' and QuantiFast SYBR Green qRT-PCR Kit (Qiagen, 204154). Separately prepared mixture of AQP5F1, AQP5R1, QuantiFast SYBR Green and TREKF1, TREKR1, QuantiFast SYBR Green was analyzed in the Rotor-Gene Q (Qiagen, Hilden, Germany). Normalising of the target genes expression changes was performed according to the ß-microtubulin (B2M) (B2MF1 5-TCTCTCTTTCTGGCCTGGA-3', B2MR1 5-TGTCGGATGGATGAAACCC-3) and Hypoxanthine Phosphoribosyl Transferase (HPRT1) (HPRT1F1 5-CGTCTTGCTCGAGATGTGAT-3', HPRT1R1 5-TTCAGTGCTTTGATGTAATCCAG-3) housekeeping gene expression values. The related forward and reverse primers were synthesized by Metabion company (Germany). qRT-PCR cycling conditions started with the reverse transcription step of 50°C (10 min), followed by PCR step comprised of an initial activation/denaturation stage of 95°C (5 min), followed by 45 cycles of denaturation 95°C (20s), combined annealing/extension 61 °C (50s). The 2^−ΔΔCT method was used to calculate the relative changes in gene expression.³¹31 Livak KJ, Schmittgen TD. Analysis of relative gene expression data using real-time quantitative PCR and the 2(-Delta Delta C(T)) Method. Methods. 2001;25:402-8.

Statistical analyses

Relative VPAC1 and VPAC2 expressions were compared between Group A and B. Distribution of data were evaluated by Shapiro-Wilk test and results were presented as mean ±Standard Deviation (SD). Variables of Group A and B were compared by independent samples t-test or Mann-Whitney U Test according to the results of Shapiro-Wilk test. The impact of serum E2 and PG levels on VPAC1 and VPAC2 was analyzed by Pearson correlation test. Statistical significance was defined as p<0.05. The Statistical Package for the Social Sciences (SPSS) Version 21.0 (IBM Corp.; Armonk, NY, USA) was used for statistical calculations.

Results

Immunohistochemistry

We observed pseudostratified cuboidal-columnar type of epithelium in Hematoxylin and Eosin (H&E) sections of nasal septal cartilage. In addition, increased superficial cellularity and sub-epithelial edema was notable in Group B when compared with the Group A (Fig. 2).

Figure 2
Septal cartilage with covering mucoperichondrium. Increased cellularity and sub-epithelial oedema is notable in pregnant group. (a) Control group (b) Pregnant group (H&E stain) (Scale Bars = 50μm and 10μm).

VPAC1 and VPAC2 were found to be located in all layers of septal specimen (epithelium, basement membrane, lamina propria, cartilage). But the staining intensity of epithelium was more distinct in specimens of both group (Figs. 3 and 4). Although we did not use an objective measure like “H-Scoring” for comparison of groups, we roughly observed higher overall staining intensity in samples of Group B when compared with Group A (Fig. 3b, Fig. 4b).

Figure 3
VPAC1 immunohistochemistry for (a) Control group and (b) Pregnant group. VPAC1 was found to be expressed in all layers of septal mucoperichondrium. Additionally, it was more intense in the surface epithelium of both groups. Overall staining intensity was more explicit in specimens of pregnant group. (Scale Bars =50μm and 10μm).

Figure 4
VPAC2 immunohistochemistry for (a) Control group and (b) Pregnant group. VPAC2 was found to be stained in all layers of septal mucoperichondrium. Subepithelial hypercellularity was remarkable in the pregnant group (b). Overall staining intensity was more explicit in specimens of pregnant group. (Scale Bars =50μm and 10μm).

PCR and ELISA

A total of 20 Wister albino female rats (10 control, 10 pregnant) were enrolled into the experiment. The mean relative expression of mRNA coding for VPAC1 of Group A and B was 0.029 ±0.016 and 0.055 ±0.026, respectively. The mean relative expression of mRNA coding for VPAC2 of Group A and B was 0.003 ± 0.001 and 0.007 ± 0.004, respectively. The mean serum E2 levels of Group A and B was 21.85±1.45pg/mL and 73.59 ± 3.01 pg/mL, respectively. The mean PG levels of Group A and Bwas14.99±1.96ng/mL and 32.80±3.96ng/mL, respectively (Table 1). PCR and ELISA values were found to be abnormally distributed (p < 0.05). For this reason, Mann-Whitney U Test was used for comparison of relative biomolecule expressions and serum sex hormone (E2, PG) levels between groups.

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Table 1
Expression of VPAC1 and VPAC2 in nasal mucosa of rat, serum E2 and PG levels based on groups.

Both relative VPAC1 (p= 0.023) and VPAC2 (p= 0.021) expression was found to be significantly higher in Group B when compared with Group A. E2 and PG were also found significantly higher in Group B when compared with Group A (p< 0.001) (Table 1).

Discussion

PR is a relatively common sex hormone-related ORL disorder. Its incidence has been reported between 10%-40%.⁸8 Ulkumen B, Ulkumen BA, Pala HG, Celik O, Sahin N, Karaca G, et al. Pregnancy rhinitis in Turkish women: Do gestational week, BMI and parity affect nasal congestion? Pak J Med Sci. 2016;32:950-4.,¹²12 Ellegård EK. Special considerations in the treatment of pregnancy rhinitis. Womens Health (Lond). 2005;1:105-14. Unfortunately, the awareness of PR among patients and even physicians is quite low. PR may cause some serious comorbidities like maternal hypertension, preeclampsia, low APGAR score and fetal growth retardation.¹⁰10 Franklin K, Holmgren PA, Jonssen F. Snoring, pregnancy-induced hypertension, and growth retardation of the fetus. Chest. 2000;117:137-41.,¹¹11 Somoskovi A, Bartfai Z, Tamasi L, Kocsis J, Puho E, Czeizel A. Population-based case-control study of allergic rhinitis during pregnancy for birth outcomes. Eur J Obstet Gynecol Reprod Biol. 2007;131:21-7.,³²32 Dzieciolowska-Baran E, Teul-Swiniarska I, Gawlikowska-Sroka A, Poziomkowska-Gesicka I, Zietek Z. Rhinitis as a cause of respiratory disorders during pregnancy. Adv Exp Med Biol. 2013;755:213-20. There are some epidemiological and physiological studies on PR,⁸8 Ulkumen B, Ulkumen BA, Pala HG, Celik O, Sahin N, Karaca G, et al. Pregnancy rhinitis in Turkish women: Do gestational week, BMI and parity affect nasal congestion? Pak J Med Sci. 2016;32:950-4.,³³33 Demir UL, Demir BC, Oztosun E, Uyaniklar OO, Ocakoglu G. The effects of pregnancy on nasal physiology. Int Forum Allergy Rhinol. 2015;5:162-6.,³⁴34 Favilli A, Laurenti E, Stagni GM, Tassi L, Ricci G, Gerli S. Effects of Sodium Hyaluronate on Symptoms and Quality of Life in Women Affected by Pregnancy Rhinitis: A Pilot Study. Gynecol Obstet Invest. 2019;84:159-65. but histopathological and biomolecular background has not been studied thoroughly. Besides, there are very limited numbers of studies regarding the treatment for this quite common disorder.¹²12 Ellegård EK. Special considerations in the treatment of pregnancy rhinitis. Womens Health (Lond). 2005;1:105-14.,³²32 Dzieciolowska-Baran E, Teul-Swiniarska I, Gawlikowska-Sroka A, Poziomkowska-Gesicka I, Zietek Z. Rhinitis as a cause of respiratory disorders during pregnancy. Adv Exp Med Biol. 2013;755:213-20.,³⁴34 Favilli A, Laurenti E, Stagni GM, Tassi L, Ricci G, Gerli S. Effects of Sodium Hyaluronate on Symptoms and Quality of Life in Women Affected by Pregnancy Rhinitis: A Pilot Study. Gynecol Obstet Invest. 2019;84:159-65.,³⁵35 Incaudo GA, Takach P. The diagnosis and treatment of allergic rhinitis during pregnancy and lactation. Immunol Allergy Clin North Am. 2006;26:137-54. Review. Suggestions for any treatment modality necessitates comprehension of physiopathology and histopathology. For this reason, in this animal experimental study, we aimed to reveal histochemical and biomolecular (VPAC1 and VPAC2) changes of nasal mucosa during gestation.

VIP plays a key role in allergic diseases like AR and asthma. It particularly functions via VPAC1 and VPAC2 in the upper respiratory tract.²³23 Abad C, Tan YV. Immunomodulatory Roles of PACAP and VIP: Lessons from Knockout Mice. J Mol Neurosci. 2018;66:102-13. Stimulation of these 2 receptors leads secretion of pro- and anti-inflammatory mediators like prostaglandins and leukotrienes. This ends up with extravasation of inflammatory cells into the mucosa. Other well-known functions of VIP are bronchodilation, vasodilation and increased glandular secretion. In addition, recent studies emphasize the neuroimmune interaction of VIP in the context of allergic diseases.²³23 Abad C, Tan YV. Immunomodulatory Roles of PACAP and VIP: Lessons from Knockout Mice. J Mol Neurosci. 2018;66:102-13.,³⁶36 Fischer A, Wussow A, Cryer A, Schmeck B, Noga O, Zweng M, et al. Neuronal plasticity in persistent perennial allergic rhinitis. J Occup Environ Med. 2005;47:20-5. All these effects may also play a role in the etiopathogenesis of PR. In fact, some researchers have been asserted that PR is caused by aggravation of preexisting subclinical allergy.³3 Kumar R, Hayhurst KL, Robson AK. Ear, nose, and throat manifestations during pregnancy. Otolaryngol Head Neck Surg. 2011;145:188-98.,¹²12 Ellegård EK. Special considerations in the treatment of pregnancy rhinitis. Womens Health (Lond). 2005;1:105-14.,¹³13 Toppozada H, Michaels L, Toppozada M, El-Ghazzawi I, Talaat M, Elwany S. The human respiratory nasal mucosa in pregnancy. An electron microscopic and histochemical study. J Laryngol Otol. 1982;96:613-26. Toppozada et al. revealed some changes like AR in specimens of PR patients by electron microscopy.¹³13 Toppozada H, Michaels L, Toppozada M, El-Ghazzawi I, Talaat M, Elwany S. The human respiratory nasal mucosa in pregnancy. An electron microscopic and histochemical study. J Laryngol Otol. 1982;96:613-26. On the other hand, Ellegard et al. revealed increased levels of IgE against house dust mite in PR patients.¹⁴14 Ellegård E, Karlsson G. IgE-mediated reactions and hyperreactivity in pregnancy rhinitis. Arch Otolaryngol Head Neck Surg. 1999;125:1121-5. In this study, we revealed a statistically significant increase of nasal VPAC1 (p= 0.023) and VPAC2 (p = 0.021) expression in pregnant rats when compared with the non-pregnant ones (Table 1). This finding supports the argument of previous researchers.¹³13 Toppozada H, Michaels L, Toppozada M, El-Ghazzawi I, Talaat M, Elwany S. The human respiratory nasal mucosa in pregnancy. An electron microscopic and histochemical study. J Laryngol Otol. 1982;96:613-26.,¹⁴14 Ellegård E, Karlsson G. IgE-mediated reactions and hyperreactivity in pregnancy rhinitis. Arch Otolaryngol Head Neck Surg. 1999;125:1121-5. In other words, this study supports the hypothesis that PR and AR may share a common pathway for VIP.

Impact of sex hormones on the nasal mucosa has been shown by previous researchers in various physiological, iatrogenic or pathological conditions.³3 Kumar R, Hayhurst KL, Robson AK. Ear, nose, and throat manifestations during pregnancy. Otolaryngol Head Neck Surg. 2011;145:188-98.,⁵5 Kabil Kucur S, Seven A, Yuksel B, Kucur C, Sencan H, Gozukara I, et al. Alterations in nasal mucociliary activity in polycystic ovary syndrome. Eur J Obstet Gynecol Reprod Biol. 2016;207:169-72.,⁶6 Bhagat DR, Chowdhary A, Verma S, Jyotsana. Physiological changes in ENT during pregnancy. Indian J Otolaryngol Head Neck Surg. 2006;58:268-70.,⁷7 Shiny Sherlie V, Varghese A. ENT Changes of Pregnancy, and Its Management. Indian J Otolaryngol Head Neck Surg. 2014;66:6-9.,¹³13 Toppozada H, Michaels L, Toppozada M, El-Ghazzawi I, Talaat M, Elwany S. The human respiratory nasal mucosa in pregnancy. An electron microscopic and histochemical study. J Laryngol Otol. 1982;96:613-26.,¹⁵15 Toppozada H. The human nasal mucosa in the menopause (a histochemical and electron microscopic study). J Laryngol Otol. 1988;102:314-8.,¹⁶16 Toppozada H, Toppozada M, El-Ghazzawi I, Elwany S. The human respiratory nasal mucosa in females using contraceptive pills. An ultramicroscopic and histochemical study. J Laryngol Otol. 1984;98:43-51.,¹⁷17 Philpott CM, Wild DC, Wolstensholme CR, Murty GE. The presence of ovarian hormone receptors in the nasal mucosa and their relationship to nasal symptoms. Rhinology. 2008;46:221-5.,¹⁸18 Horie S, Yamaki A, Takami S. Presence of Sex Steroid-Metabolizing Enzymes in the Olfactory Mucosa of Rats. Anat Rec (Hoboken). 2017;300:402-14.,¹⁹19 Karaer I, Tuncay G. The effect of premature ovarian insufficiency on nasal mucociliary clearance time. Gynecol Endocrinol. 2019;25:1-4.,²⁰20 Konno A, Terada N, Okamoto Y Effects of female hormones on the muscarinic and alpha 1-adrenergic receptors of the nasal mucosa. An experimental study in guinea pigs. ORL J Otorhinolaryngol Relat Spec. 1986;48:45-51.,²¹21 Orban N, Maughan E, Bleach N. Pregnancy-induced rhinitis. Rhinology. 2013;51:111-9.,²²22 Verma AK, Manohar M, Upparahalli Venkateshaiah S, Mishra A. Neuroendocrine cells derived chemokine Vasoactive Intestinal Polypeptide (VIP) in allergic diseases. Cytokine Growth Factor Rev. 2017;38:37-48. Almost all concluded that E2 and PG causes obstruction and edema in the nasal cavity which is the case in this study (Fig. 2b).³3 Kumar R, Hayhurst KL, Robson AK. Ear, nose, and throat manifestations during pregnancy. Otolaryngol Head Neck Surg. 2011;145:188-98.,⁶6 Bhagat DR, Chowdhary A, Verma S, Jyotsana. Physiological changes in ENT during pregnancy. Indian J Otolaryngol Head Neck Surg. 2006;58:268-70.,¹³13 Toppozada H, Michaels L, Toppozada M, El-Ghazzawi I, Talaat M, Elwany S. The human respiratory nasal mucosa in pregnancy. An electron microscopic and histochemical study. J Laryngol Otol. 1982;96:613-26.,¹⁵15 Toppozada H. The human nasal mucosa in the menopause (a histochemical and electron microscopic study). J Laryngol Otol. 1988;102:314-8.,¹⁶16 Toppozada H, Toppozada M, El-Ghazzawi I, Elwany S. The human respiratory nasal mucosa in females using contraceptive pills. An ultramicroscopic and histochemical study. J Laryngol Otol. 1984;98:43-51.,²¹21 Orban N, Maughan E, Bleach N. Pregnancy-induced rhinitis. Rhinology. 2013;51:111-9. In addition to these findings, we found a relatively increased superficial higher cellularity in the epithelial layer in samples of Group B. This may be a sign of increased metabolism or activity. On the other hand, very few researchers evaluate the underlying histochemical and biomolecular changes. Konno et al. revealed that E2 up-regulates cholinergic muscarinic receptors while PG down-regulates α1 -adrenergic receptors.²⁰20 Konno A, Terada N, Okamoto Y Effects of female hormones on the muscarinic and alpha 1-adrenergic receptors of the nasal mucosa. An experimental study in guinea pigs. ORL J Otorhinolaryngol Relat Spec. 1986;48:45-51. These findings of Konno et al. are compatible with the study of Fisher et al. in relation to neuroimmunomodulation.³⁶36 Fischer A, Wussow A, Cryer A, Schmeck B, Noga O, Zweng M, et al. Neuronal plasticity in persistent perennial allergic rhinitis. J Occup Environ Med. 2005;47:20-5. Fisher et al. revealed higher VIP contents in mucosal nerve fibers of AR patients when compared with control. Our findings also support this phenomenon. The higher nasal VPAC1 and VPAC2 expression in pregnancy that was revealed in this study can also be the triggering factor for PR. Besides, Philpott et al. discovered a positive correlation between oestrogen-β (ERβ) receptor expression and rhinitis symptoms.¹⁷17 Philpott CM, Wild DC, Wolstensholme CR, Murty GE. The presence of ovarian hormone receptors in the nasal mucosa and their relationship to nasal symptoms. Rhinology. 2008;46:221-5. Our findings also support this correlation. We revealed up-regulatory effect of E2 and PG on VPAC1 by PCR. But VPAC2 was found to be stimulated only by E2. These findings may be the missing link of the VIP pathway triggered by sex hormones, resulting in extravasation of inflammatory cells into the nasal mucosa.

In the current study, both VPAC1 and VPAC2 were found to be located in all layers of septal mucoperichondrium. However, the surface epithelium of both groups demonstrated higher immunostaining for both VIP receptors. In addition, we revealed higher overall staining intensity in samples of pregnant rats (Figs. 3 and 4). These IHC findings are similar to the study of Kim et al.²⁵25 Voice JK, Dorsam G, Lee H, Kong Y Goetzl EJ. Allergic diathesis in transgenic mice with constitutive T-cell expression of inducible vasoactive intestinal peptide receptor. FASEB J. 2001;15:2489-96. They demonstrated increased staining intensity for VIP receptors in nasal mucosa of AR patients. Therefore, we can suggest that PR and AR have a similar effect on VIP receptors. On the other hand, this strong immunostaining particularly demonstrated in the surface epithelium can be interpreted as a sign of hyper responsiveness of nasal mucosa in pregnancy.

Conclusions

We revealed gestational upregulation of VPAC1 and VPAC2 expression in rat nasal mucosa for the first time both by PCR and IHC. The current study supports the hypothesis that PR is caused by the activation of a subclinical allergy that is present before pregnancy. Further studies are needed to unveil the complete histopathological and biomolecular changes regarding PR.

Ethical approval

This animal experimental research was approved by the Laboratory Animals Local Ethics Committee of Manisa Celal Bayar University (28.04.2015/77.637.435-29) and was performed in institutional Experimental Animals Research and Application Center in accordance with the accepted policy on the use of animals.

Committee Name: The Laboratory Animals Local Ethics Committee of Manisa Celal Bayar University. Permit number: (28.04.2015/77.637.435-29).
Funding

Unit of Scientific Research Projects (BAP) of Manisa Celal Bayar University (Grant number: 2014-131).
Peer Review under the responsibility of Associação Brasileira de Otorrinolaringologia e Cirurgia Cérvico-Facial.

References

¹
D’haeseleer E, Depypere H, Claeys S, Van Borsel J, Van Lierde K. The menopause and the female larynx, clinical aspects, and therapeutic options: a literature review. Maturitas. 2009;64:27-32.
²
Turan M, Ucler R, Garca MF, Kurdoglu Z, Cankaya H, Ayral A, et al. The Relationship Between Hearing Thresholds and Hyperandrogenism in Polycystic Ovary Syndrome. Med Sci Monit. 2016;22:4380-5.
³
Kumar R, Hayhurst KL, Robson AK. Ear, nose, and throat manifestations during pregnancy. Otolaryngol Head Neck Surg. 2011;145:188-98.
⁴
Shoffel-Havakuk H, Carmel-Neiderman NN, Halperin D, Shapira Galitz Y Levin D, Haimovich Y, et al. Menstrual Cycle, Vocal Performance, and Laryngeal Vascular Appearance: An Observational Study on 17 Subjects. J Voice. 2018;32:226-33.
⁵
Kabil Kucur S, Seven A, Yuksel B, Kucur C, Sencan H, Gozukara I, et al. Alterations in nasal mucociliary activity in polycystic ovary syndrome. Eur J Obstet Gynecol Reprod Biol. 2016;207:169-72.
⁶
Bhagat DR, Chowdhary A, Verma S, Jyotsana. Physiological changes in ENT during pregnancy. Indian J Otolaryngol Head Neck Surg. 2006;58:268-70.
⁷
Shiny Sherlie V, Varghese A. ENT Changes of Pregnancy, and Its Management. Indian J Otolaryngol Head Neck Surg. 2014;66:6-9.
⁸
Ulkumen B, Ulkumen BA, Pala HG, Celik O, Sahin N, Karaca G, et al. Pregnancy rhinitis in Turkish women: Do gestational week, BMI and parity affect nasal congestion? Pak J Med Sci. 2016;32:950-4.
⁹
Ayrim A, Keskin E, Ozol D, Onaran Y Yidirim Z, Kafali H. Influence of self-reported snoring and witnessed sleep apnea on gestational hypertension and fetal outcome in pregnancy. Arch Gynecol Obstet. 2011;283:195-9.
¹⁰
Franklin K, Holmgren PA, Jonssen F. Snoring, pregnancy-induced hypertension, and growth retardation of the fetus. Chest. 2000;117:137-41.
¹¹
Somoskovi A, Bartfai Z, Tamasi L, Kocsis J, Puho E, Czeizel A. Population-based case-control study of allergic rhinitis during pregnancy for birth outcomes. Eur J Obstet Gynecol Reprod Biol. 2007;131:21-7.
¹²
Ellegård EK. Special considerations in the treatment of pregnancy rhinitis. Womens Health (Lond). 2005;1:105-14.
¹³
Toppozada H, Michaels L, Toppozada M, El-Ghazzawi I, Talaat M, Elwany S. The human respiratory nasal mucosa in pregnancy. An electron microscopic and histochemical study. J Laryngol Otol. 1982;96:613-26.
¹⁴
Ellegård E, Karlsson G. IgE-mediated reactions and hyperreactivity in pregnancy rhinitis. Arch Otolaryngol Head Neck Surg. 1999;125:1121-5.
¹⁵
Toppozada H. The human nasal mucosa in the menopause (a histochemical and electron microscopic study). J Laryngol Otol. 1988;102:314-8.
¹⁶
Toppozada H, Toppozada M, El-Ghazzawi I, Elwany S. The human respiratory nasal mucosa in females using contraceptive pills. An ultramicroscopic and histochemical study. J Laryngol Otol. 1984;98:43-51.
¹⁷
Philpott CM, Wild DC, Wolstensholme CR, Murty GE. The presence of ovarian hormone receptors in the nasal mucosa and their relationship to nasal symptoms. Rhinology. 2008;46:221-5.
¹⁸
Horie S, Yamaki A, Takami S. Presence of Sex Steroid-Metabolizing Enzymes in the Olfactory Mucosa of Rats. Anat Rec (Hoboken). 2017;300:402-14.
¹⁹
Karaer I, Tuncay G. The effect of premature ovarian insufficiency on nasal mucociliary clearance time. Gynecol Endocrinol. 2019;25:1-4.
²⁰
Konno A, Terada N, Okamoto Y Effects of female hormones on the muscarinic and alpha 1-adrenergic receptors of the nasal mucosa. An experimental study in guinea pigs. ORL J Otorhinolaryngol Relat Spec. 1986;48:45-51.
²¹
Orban N, Maughan E, Bleach N. Pregnancy-induced rhinitis. Rhinology. 2013;51:111-9.
²²
Verma AK, Manohar M, Upparahalli Venkateshaiah S, Mishra A. Neuroendocrine cells derived chemokine Vasoactive Intestinal Polypeptide (VIP) in allergic diseases. Cytokine Growth Factor Rev. 2017;38:37-48.
²³
Abad C, Tan YV. Immunomodulatory Roles of PACAP and VIP: Lessons from Knockout Mice. J Mol Neurosci. 2018;66:102-13.
²⁴
Kim DH, Park IH, Cho JS, Lee YM, Choi H, Lee HM. Alterations of vasoactive intestinal polypeptide receptors in allergic rhinitis. Am J Rhinol Allergy. 2011;25:44-7.
²⁵
Voice JK, Dorsam G, Lee H, Kong Y Goetzl EJ. Allergic diathesis in transgenic mice with constitutive T-cell expression of inducible vasoactive intestinal peptide receptor. FASEB J. 2001;15:2489-96.
²⁶
Samarasinghe AE, Hoselton SA, Schuh JM. The absence of VPAC2 leads to aberrant antibody production in Aspergillus fumigatus sensitized and challenged mice. Peptides. 2011;32:131-7.
²⁷
Agematsu Y Ikadai H, Amao H. Early detection of pregnancy of the rat. Jikken Dobutsu. 1983;32:209-12.
²⁸
Lohmiller JJ, Swing SP. Reproduction and Breeding. In: Suckow MA, Weisbroth SH, Franklin CL, editors. The laboratory rat. Boston BOS. Elsevier; 2006. p. 147-65.
²⁹
Ulkumen B, Artunc Ulkumen B, Batir MB, Pala HG, Vatansever S, Cam S. Impact of Pregnancy and Glucocorticoid Treatment on NF-KB and MUC5AC in Mucosa of Rat Larynx. J Voice. 2021;35:342-8.
³⁰
Alvites RD, Caseiro AR, Pedrosa SS, Branquinho ME, Varejão ASP, Maurício AC. The Nasal Cavity of the Rat and Mouse-Source of Mesenchymal Stem Cells for Treatment of Peripheral Nerve Injury. Anat Rec (Hoboken). 2018;301:1678-89.
³¹
Livak KJ, Schmittgen TD. Analysis of relative gene expression data using real-time quantitative PCR and the 2(-Delta Delta C(T)) Method. Methods. 2001;25:402-8.
³²
Dzieciolowska-Baran E, Teul-Swiniarska I, Gawlikowska-Sroka A, Poziomkowska-Gesicka I, Zietek Z. Rhinitis as a cause of respiratory disorders during pregnancy. Adv Exp Med Biol. 2013;755:213-20.
³³
Demir UL, Demir BC, Oztosun E, Uyaniklar OO, Ocakoglu G. The effects of pregnancy on nasal physiology. Int Forum Allergy Rhinol. 2015;5:162-6.
³⁴
Favilli A, Laurenti E, Stagni GM, Tassi L, Ricci G, Gerli S. Effects of Sodium Hyaluronate on Symptoms and Quality of Life in Women Affected by Pregnancy Rhinitis: A Pilot Study. Gynecol Obstet Invest. 2019;84:159-65.
³⁵
Incaudo GA, Takach P. The diagnosis and treatment of allergic rhinitis during pregnancy and lactation. Immunol Allergy Clin North Am. 2006;26:137-54. Review.
³⁶
Fischer A, Wussow A, Cryer A, Schmeck B, Noga O, Zweng M, et al. Neuronal plasticity in persistent perennial allergic rhinitis. J Occup Environ Med. 2005;47:20-5.

Publication Dates

Publication in this collection
15 Aug 2022
Date of issue
Jul-Aug 2022

History

Received
13 Jan 2020
Accepted
28 June 2020
Published
01 Aug 2020

This is an Open Access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.

[1] Ethical approval

This animal experimental research was approved by the Laboratory Animals Local Ethics Committee of Manisa Celal Bayar University (28.04.2015/77.637.435-29) and was performed in institutional Experimental Animals Research and Application Center in accordance with the accepted policy on the use of animals.

Committee Name: The Laboratory Animals Local Ethics Committee of Manisa Celal Bayar University. Permit number: (28.04.2015/77.637.435-29).

[2] Funding

Unit of Scientific Research Projects (BAP) of Manisa Celal Bayar University (Grant number: 2014-131).

[3] Peer Review under the responsibility of Associação Brasileira de Otorrinolaringologia e Cirurgia Cérvico-Facial.

Biomolecules & sex hormones	Control (Group A)	Pregnant (Group B)	p-value^a ap-values obtained by Mann-Whitney U Test.
Biomolecules
VPAC1 (REV)	0.029±0.016	0.055±0.026	p = 0.023
VPAC2 (REV)	0.003 ±0.001	0.007 ±0.004	p = 0.021
Serum sex hormone levels
Estradiol (pg/mL)	21.85±1.45pg	73.59 ± 3.01 pg/mL	p<0.001
Progesterone (ng/mL)	14,99 ± 1.96ng/mL	32.80±3.96ng/mL	p<0.001

Brasil