September 26-27, 2014
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Abstract Details9/26/2014 | 4:30 PM - 6:00 PM | Protection of placental stem cells against CMV infection by human monoclonal antibodies Human cytomegalovirus (CMV) is the leading cause of congenital infection and affects 1%-3% of births in the United States. The risk of transplacental transmission upon primary maternal infection in the first trimester of pregnancy is high (40-50%) and symptomatic babies can have permanent birth defects, such as neurological deficiencies and deafness. The molecular mechanisms that govern congenital CMV infection and disease are largely unknown. With regard to the maternal-fetal interface, it is now believed that upon placental infection CMV dysregulates the development of chorionic villi, resulting in functional defects that reduce transport of substances from the mother to the fetus. Trophoblast stem cells (TBPCs) are essential for the normal development of chorionic villi, being the only source of cells that can differentiate to form the mature cell populations of syncytiotrophoblasts and cytotrophoblasts. Our recent research revealed that TBPCs can be infected with CMV and that the cells support the entire lytic infectious cycle of the virus, leading to the release of progeny virions. In addition, infection inhibits the differentiation of TBPCs. Important for future interventions, CMV infection of TBPCs can be prevented by highly potent neutralizing antibodies to glycoprotein B (gB) but not by antibodies, which target another viral surface protein complex known as the pentamer complex. Virus neutralization with anti-gB proved to be sufficient to preserve the ability of TBPCs to differentiate. Our data indicate that – in order to be broadly effective – a future preventative treatment based on monoclonal antibodies should not exclusively target the viral pentamer complex but also gB. Our research was supported by NIAID RO1AI046657, R56AI21739 (L.P.), R44AI102396 (L.K.); and DFG ZY110/1-1 (M.Z.).
Martin Zydek (Primary Presenter), martin.zydek@ucsf.edu;
ASHA DISCLOSURE:
Takako Tabata (Co-Presenter), takako.tabata@ucsf.edu;
ASHA DISCLOSURE:
Matthew Petitt (Co-Presenter), matthew.petitt@ucsf.edu;
ASHA DISCLOSURE:
June Fang-Hoover (Co-Presenter), june.fang-hoover@ucsf.edu;
ASHA DISCLOSURE:
Lawrence M Kauvar (Co-Presenter), lkauvar@trellisbio.com;
ASHA DISCLOSURE:
Lenore Pereira (Co-Presenter), lenore.pereira@ucsf.edu;
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