Intranasal infection and contact transmission of Zika virus in guinea pigs

Deng, Yong-Qiang; Zhang, Nana; Li, Xiaofeng; Wang, Yaqing; Tian, Min; Qiu, Yefeng; Fan, Junwan; Hao, Jia; Huang, Xing‐Yao; Dong, Hao-Long; Fan, Hang; Wang, Yuguang; Zhang, Fuchun; Tong, Yigang; Xu, Zhiheng; Qin, Cheng‐Feng

doi:10.1038/s41467-017-01923-4

Cited by 45 publications

(71 citation statements)

References 51 publications

(59 reference statements)

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“…However, the explosive growth of ZIKV research since 2015 has spurred the development of new animal models, revealing pathogenic mechanisms and providing systems for evaluating therapeutic interventions. The most significant models of ZIKV infection are non-human primates and mice (7), but ZIKV disease also has been studied in guinea pigs, hamsters, tree shrews, and swine (27-35). Mice offer significant advantages in terms of cost, scale, speed, and genetic tractability, enabling mechanistic studies that are not feasible in non-human primate models.…”

Section: Discussionmentioning

confidence: 99%

Zika virus infection in Collaborative Cross mice

Mattocks

Plante

Fritch

et al. 2019

Preprint

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14The 2015-2016 emergence of Zika virus (ZIKV) in the Americas, and recognition that ZIKV 15 infection during pregnancy can result in birth defects, revealed a need for small animal models to 16 study ZIKV pathogenic mechanisms and evaluate candidate vaccines and antivirals. Mice would 17 be an attractive system for such studies, but ZIKV replicates poorly in laboratory mice because it 18 fails to antagonize murine STAT2 and STING. To address this, most ZIKV pathogenesis studies 19 have used mice with impaired interferon signaling (e.g. Ifnar1 -/or treatment with IFNAR1-blocking 20 antibodies). However, using mice with severe defects in innate antiviral signaling confounds 21 studies of viral pathogenic mechanisms. Collaborative Cross (CC) mice have proven to be a 22valuable system for developing new mouse pathogenesis models for viral infections that are not 23 well modeled in conventional laboratory mouse lines. To test whether CC mice could provide an 24 immune-competent model for ZIKV pathogenesis, we infected CC lines with ZIKV and assessed 25 weight loss, viremia, and production of neutralizing antibodies. We tested 21 CC lines (CC001, 26 All rights reserved. No reuse allowed without permission.

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Section: Discussionmentioning

confidence: 99%

Zika virus infection in Collaborative Cross mice

Mattocks

Plante

Fritch

et al. 2019

Preprint

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“…Several other animal models have been used to study ZIKV but most are not focused on sexual transmission. These models include guinea pigs [109][110][111], hamsters [112], bats [113], chick embryos, piglets [114,115] and boars [116]. Porcine fetuses were shown to present mild to severe neuropathology upon ZIKV infection [114,115].…”

Section: Other Animal Modelsmentioning

confidence: 99%

“…One study with ZIKV challenge mid-gestation showed no evidence of infection [109]; however, Kumar et al show guinea pigs inoculated subcutaneously with PRVABC59 had viremia and presented signs such as fever, hunched posture and detectable viral RNA in the blood [110]. Deng et al showed that intranasally-infected guinea pigs have virus in the sera, saliva and tears [111].…”

Section: Other Animal Modelsmentioning

confidence: 99%

Animal Models of Zika Virus Sexual Transmission

Campos¹,

McDonald²,

Brault³

et al. 2021

Current Concepts in Zika Research

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ZIKV was first identified in the 1940s as a mosquito-borne virus; however, sexual transmission, which is uncommon for arboviruses, was demonstrated more than 60 years later. Tissue culture and animal models have allowed scientists to study how this transmission is possible. Immunocompromised mice infected with ZIKV had high viral loads in their testes, and infection of immunocompetent female mice was achieved following intravaginal inoculation or inoculation via mating with an infected male. These mouse studies lead researchers to investigate the individual components of the male reproductive system. In cell culture and mouse models, ZIKV can persist in Sertoli and germ cells of the testes and epithelial cells in the epididymis, which may lead to sexual transmission even after ZIKV has been cleared from other tissues. ZIKV has also been studied in nonhuman primates (NHPs), which appears to mimic the limited human epidemiological data, with low rates of symptomatic individuals and similar clinical signs. Although refinement is needed, these animal models have proven to be key in ZIKV research and continue to help uncovering the mechanisms of sexual transmission. This review will focus on the animal models used to elucidate the mechanisms of sexual transmission and persistence of flaviviruses.

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“…Guinea pigs have also been intranasally infected with ZIKA virus (ZIKAV). Nasal infection with ZIKAV results in infection of the brain, parotid glands, tears, saliva and sera but NALT immune responses were not evaluated (Deng et al, 2017). Of interest, nasal vaccination of guinea pigs with a genital herpesvirus HSV2 vaccine results in protection to genital herpes and elicits systemic specific IgG but not IgA titers (Persson et al, 2016).…”

Section: Rats and Guinea Pigs As Models Of Human Nasal Diseasesmentioning

confidence: 99%

“…After 7 days post inoculation, IgM and IgA antibodies were detected, followed by IgG. Thus, a strong infection in the nasal mucosa was established in A129 mice (Deng et al, 2017). A vaccine against the envelope protein E of ZIKAV was tested in this mouse strain and production of neutralizing antibodies was able to confer protection against ZIKAV and other Flaviviridae (Sumathy et al, 2017).…”

Section: Mouse Models Of Human Nasal Diseases: What Are the Limitations?mentioning

confidence: 99%