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Mouse Model For Zika - ASTMH


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  1. Scott C. Weaver

-Author Affiliations

  1. Institute for Human Infections and Immunity, University of Texas Medical Branch, Galveston, Texas; Department of Pathology, University of Texas Medical Branch, Galveston, Texas; Institute for Translational Science, University of Texas Medical Branch, Galveston, Texas; Department of Microbiology and Immunology, University of Texas Medical Branch, Galveston, Texas; Sealy Center for Vaccine Development, University of Texas Medical Branch, Galveston, Texas; Department of Biology, New Mexico State University, Las Cruces, New Mexico

-Author Notes

  • Authors' addresses: Shannan L. Rossi, Robert B. Tesh, Albert J. Auguste, Slobodan Paessler, and Nikos Vasilakis, Institute of Human Infection and Immunity University of Texas Medical Branch, Galveston, TX, and Department of Pathology, University of Texas Medical Branch, Galveston, TX, E-mails: [email protected],[email protected][email protected][email protected], and[email protected]. Sasha R. Azar and Rose M. Langsjoen, Institute for Translational Studies, University of Texas Medical Branch, Galveston, TX, E-mails: [email protected] and [email protected]. Antonio E. Muruato, Department of Microbiology and Immunology, University of Texas Medical Branch, Galveston, TX, E-mail:[email protected]. Kathryn A. Hanley, Department of Biology, New Mexico State University, Las Cruces, NM, E-mail:[email protected]. Scott C. Weaver, Institute of Human Infection and Immunity, University of Texas Medical Branch, Galveston, TX, Sealy Center for Vaccine Development, University of Texas Medical Branch, Galveston, TX, and Department of Microbiology and Immunology, University of Texas Medical Branch, Galveston, TX, E-mail: [email protected].

  1. * Address correspondence to Shannan L. Rossi, Department of Pathology, University of Texas Medical Branch, 301 University Boulevard, Galveston, TX 77555-0609. E-mail: [email protected]
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Abstract

The mosquito-borne Zika virus (ZIKV) is responsible for an explosive ongoing outbreak of febrile illness across the Americas. ZIKV was previously thought to cause only a mild, flu-like illness, but during the current outbreak, an association with Guillain–Barré syndrome and microcephaly in neonates has been detected. A previous study showed that ZIKV requires murine adaptation to generate reproducible murine disease. In our study, a low-passage Cambodian isolate caused disease and mortality in mice lacking the interferon (IFN) alpha receptor (A129 mice) in an age-dependent manner, but not in similarly aged immunocompetent mice. In A129 mice, viremia peaked at ∼107plaque-forming units/mL by day 2 postinfection (PI) and reached high titers in the spleen by day 1. ZIKV was detected in the brain on day 3 PI and caused signs of neurologic disease, including tremors, by day 6. Robust replication was also noted in the testis. In this model, all mice infected at the youngest age (3 weeks) succumbed to illness by day 7 PI. Older mice (11 weeks) showed signs of illness, viremia, and weight loss but recovered starting on day 8. In addition, AG129 mice, which lack both type I and II IFN responses, supported similar infection kinetics to A129 mice, but with exaggerated disease signs. This characterization of an Asian lineage ZIKV strain in a murine model, and one of the few studies reporting a model of Zika disease and demonstrating age-dependent morbidity and mortality, could provide a platform for testing the efficacy of antivirals and vaccines.

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PUBLIC RELEASE: 

New mouse model for Zika virus to enable immediate screening of potential drugs and vaccines

Research in American Journal of Tropical Medicine and Hygiene describes first new Zika animal model in decades

BURNESS COMMUNICATIONS

Oakbrook Terrace, Ill. (March 28, 2016)-- Efforts to combat the rapid spread of Zika virus got a boost this week as researchers at the University of Texas Medical Branch, Galveston (UTMB) announced the first peer-reviewed publication of a mouse model for Zika infection reported in decades. Several research institutions and companies have vaccine and drug candidates nearly ready to test, but until now a mouse model - a critical stage in preclinical testing - has not been available. The study, published in the American Journal of Tropical Medicine and Hygiene (AJTMH), removes a bottleneck that was delaying treatment screening.

"There is a huge demand to screen antivirals that have been backlogged because we haven't had a good way to test them," said Shannan Rossi, PhD, a UTMB virologist and lead author of the study. "Without this model, we were really stagnant in our efforts to find new treatments. You can look for efficacy in cell cultures, but that tells you almost nothing about what's going to happen when you test in a mouse or a human. This will help get those drug and vaccine candidates moving through the pipeline."

Rossi and UTMB colleague Scott Weaver, PhD, a virologist and vector biologist, have been on the forefront of investigations into the meteoric rise in Zika virus infection raging through Central and South America. Weaver, an expert in mosquito-borne viruses in the family that includes Zika, dengue, West Nile and yellow fever, warned as early as 2009 that Zika presented a threat in the Americas. With an epidemic underway, the race is on to rapidly develop new treatments.

"Normally, creating a mouse model like this would take us several months, but the urgency of the situation propelled us into this rapid response, and we were able to put together our results in just three weeks," Rossi said.

Using funding from a grant to the World Reference Center for Emerging Viruses and Arboviruses (WRCEVA) at UTMB, Rossi injected several genetically distinct varieties of laboratory mice with Zika virus isolated in Asia in 2010. The current epidemic in South America can be traced to the Asian Zika virus lineage, of which this strain is a member.

Normal mice did not develop disease after infection with Zika virus, the research team reported. Only when researchers injected mice that had been genetically altered to have a deficient innate immune response did the animals develop detectible disease. Young mice of these strains are highly susceptible to infection. These mice became lethargic, lost weight and died within six days after infection. Older mice became ill, but did not always develop infection, and they ultimately recovered.

The mouse model is available immediately for testing of antivirals, and Weaver said that preliminary testing is already underway with an antiviral developed by another member of the UTMB team, Pei-Yong Shi, PhD, to treat dengue fever.

Since so little is known about how Zika virus behaves once inside the body, researchers also searched for evidence of viral infection in the animals' organs. They found viral particles in most of the major organ systems, with the highest levels found in the spleen, brain and testes. While the results are preliminary, the findings corroborate evidence that the virus can be sexually transmitted. The finding of virus in the brain could also be important, since the most devastating impact of the current outbreak in Brazil appears to be children of infected mothers born with microcephaly - abnormally small heads and, in some cases, incomplete brain development.

While the mouse study does not prove a direct connection between Zika infection and microcephaly, Rossi said, it does underscore the urgent need for effective animal models to further study the course of disease and its transmission.

The mice described in the current report were developed for testing of drug and vaccine candidates and may not be good models for human transmission, said Weaver.

Understanding human transmission will likely require non-human primate models and UTMB is also working on that research, he added, although all of these studies are in the early stages.

He emphasized that the bulk of research on Zika virus was published in the 1950s and 1960s. And until media attention surged recently, there had been little interest or research funding available to study Zika virus. Thus, there is limited knowledge about the extent and mechanisms of transmission during the current outbreak in the Americas and even less about how the virus is circulating in Asia. The difficulty in tracking Zika stems from the fact that most people who become infected show no symptoms at all, and those who do become ill have signs and symptoms that overlap with more common viral infections, such as dengue and chikungunya. Further, current serologic tests often can't distinguish between related flavivirus infections in dengue-endemic regions. Ongoing, long-term funding is necessary to be better prepared for these types of outbreaks, he said.

The Aedes aegypti mosquitoes that are believed to spread Zika virus can be found all over the southern United States. With the rainy season approaching in Central America and the Caribbean, Weaver said transmission is likely to pick up, and more travel-related cases may be reported in the United States.

"There's a risk from every one of those travel-related cases," said Weaver. "Most of them will not lead to local transmission, but our experience with dengue and chikungunya tells us that some of them probably will."

"This research team's dedication and previous research on dengue and other arboviruses enabled them to quickly develop this model for Zika virus, an important first step to enable testing of candidate vaccine and therapeutics," said Stephen Higgs, PhD, the president of the American Society of Tropical Medicine and Hygiene. "The lack of research on Zika virus in the decades since it was discovered and the current epidemic reveals our vulnerability to these poorly understood viruses and demonstrates the need for smart and, more importantly, sustained investments to support basic and applied research."

###

About the American Society of Tropical Medicine and Hygiene

The American Society of Tropical Medicine and Hygiene, founded in 1903, is the largest international scientific organization of experts dedicated to reducing the worldwide burden of tropical infectious diseases and improving global health. We accomplish this through generating and sharing scientific evidence, informing health policies and practices, fostering career development, recognizing excellence, and advocating for investment in tropical medicine/global health research. For more information, visit http://www.astmh.org

About the American Journal of Tropical Medicine and Hygiene

Continuously published since 1921, AJTMH is the peer-reviewed journal of the American Society of Tropical Medicine and Hygiene, and the world's leading voice in the fields of tropical medicine and global health. AJTMH disseminates new knowledge in fundamental, translational, clinical and public health sciences focusing on improving global health.

http://www.eurekalert.org/pub_releases/2016-03/bc-nmm032316.php

 

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LOCUS       JN860885               10269 bp    RNA     linear   VRL 19-MAR-2012
DEFINITION  Zika virus isolate FSS13025 polyprotein gene, partial cds.
ACCESSION   JN860885
VERSION     JN860885.1  GI:380036385
KEYWORDS    .
SOURCE      Zika virus
  ORGANISM  Zika virus
            Viruses; ssRNA viruses; ssRNA positive-strand viruses, no DNA
            stage; Flaviviridae; Flavivirus.
REFERENCE   1  (bases 1 to 10269)
  AUTHORS   Haddow,A.D., Schuh,A.J., Yasuda,C.Y., Kasper,M.R., Heang,V.,
            Huy,R., Guzman,H., Tesh,R.B. and Weaver,S.C.
  TITLE     Genetic characterization of zika virus strains: geographic
            expansion of the asian lineage
  JOURNAL   PLoS Negl Trop Dis 6 (2), E1477 (2012)
   PUBMED   22389730
  REMARK    Publication Status: Online-Only
REFERENCE   2  (bases 1 to 10269)
  AUTHORS   Haddow,A.D. and Schuh,A.J.
  TITLE     Direct Submission
  JOURNAL   Submitted (17-OCT-2011) Department of Pathology, University of
            Texas Medical Branch, 301 University Blvd, Galveston, TX 77555, USA
FEATURES             Location/Qualifiers
     source          1..10269
                     /organism="Zika virus"
                     /mol_type="genomic RNA"
                     /isolate="FSS13025"
                     /host="Homo sapiens"
                     /db_xref="taxon:64320"
                     /country="Cambodia"
                     /collection_date="2010"
                     /note="Passage History: Vero African green monkey kidney
                     cells 1 time;
                     serogroup: Spondweni"

http://www.ncbi.nlm.nih.gov/nuccore/JN860885

 

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