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Dive into the research topics where Ching-Juh Lai is active.

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Featured researches published by Ching-Juh Lai.


Journal of Virology | 2009

Passage of Dengue Virus Type 4 Vaccine Candidates in Fetal Rhesus Lung Cells Selects Heparin-Sensitive Variants That Result in Loss of Infectivity and Immunogenicity in Rhesus Macaques

Germán Añez; Ruhe Men; Kenneth H. Eckels; Ching-Juh Lai

ABSTRACT Three dengue virus type 4 (DENV-4) vaccine candidates containing deletions in the 3′ noncoding region were prepared by passage in DBS-FRhL-2 (FRhL) cells. Unexpectedly, these vaccine candidates and parental DENV-4 similarly passaged in the same cells failed to elicit either viremia or a virus-neutralizing antibody response. Consensus sequence analysis revealed that each of the three viruses, as well as the parental DENV-4 when passaged in FRhL cells, rapidly acquired a single Glu327-Gly substitution in domain III (DIII) of the envelope protein (E). These variants appear to have accumulated in response to growth adaptation to FRhL cells as shown by growth analysis, and the mutation was not detected in the virus following passage in C6/36 cells, primary African green monkey kidney cells, or Vero cells. The Glu327-Gly substitution was predicted by molecular modeling to increase the net positive charge on the surface of E. The Glu327-Gly variant of the full-length DENV-4 selected after three passages in FRhL cells showed increased affinity for heparan sulfate compared to the unpassaged DENV-4, as measured by heparin binding and infectivity inhibition assays. Evidence indicates that the Glu327-Gly mutation in DIII of the DENV-4 E protein was responsible for reduced infectivity and immunogenicity in rhesus monkeys. Our results point out the importance of cell substrates for vaccine preparation since the virus may change during passages in certain cells through adaptive selection, and such mutations may affect cell tropism, virulence, and vaccine efficacy.


Archive | 1992

Chimeric and/or growth-restricted flaviviruses

Ching-Juh Lai; Michael Bray; Alexander G. Pletnev; Ruhe Men; Yi-Ming Zhang; Kenneth H. Eckels; Robert Chanock


Journal of Virology | 1996

Monkeys immunized with intertypic chimeric dengue viruses are protected against wild-type virus challenge.

Michael Bray; Ruhe Men; Ching-Juh Lai


Archive | 1998

Chimeric vaccine against tick-borne encephalitis virus

Alexander G. Pletnev; Ruhe Men; Robert Chanock; Ching-Juh Lai


Archive | 2016

Cloning DNA sequences from influenza viral RNA segments (cDNA strands/cleavage maps/nonstructural protein/matrix protein/hemagglutinin)

Ching-Juh Lai; Lewis Markoff; Susan Zimmerman; Bronna Cohen; Jo Ann Berndt; Robert M. Chanock


Archive | 1998

Chimäres vakzin gegen das zeckenenzephalitis virus

Robert Chanock; Ching-Juh Lai; Ruhe Men; Alexander G. Pletnev


Archive | 1998

Vaccin chimere contre le virus de l'encephalite transmis par les tiques

Robert Chanock; Ching-Juh Lai; Ruhe Men; Alexander G. Pletnev


Archive | 1998

Chimeric vaccine against the tick encephalitis virus

Alexander G. Pletnev; Ruhe Men; Robert Chanock; Ching-Juh Lai


Archive | 1998

Chimärer impfstoff gegen das zeckenenzephalitis virus Chimeric vaccine against the tick encephalitis virus

Alexander G. Pletnev; Ruhe Men; Robert Chanock; Ching-Juh Lai


Archive | 1992

Chimäre und/oder wachstumsgehemmte flaviviren Chimeric and / or growth-inhibited flaviviruses

Ching-Juh Lai; Michael Bray; G Pletnev; Ruhe Men; M Chanock

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Ruhe Men

National Institutes of Health

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Alexander G. Pletnev

National Institutes of Health

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Michael Bray

National Institutes of Health

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Kenneth H. Eckels

Walter Reed Army Institute of Research

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Germán Añez

Center for Biologics Evaluation and Research

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Jo Ann Berndt

National Institutes of Health

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Lewis Markoff

National Institutes of Health

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Robert M. Chanock

National Institutes of Health

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Yi-Ming Zhang

National Institutes of Health

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