Antigenic Structure of Transmissible Gastroenteritis Virus. I. Properties of Monoclonal Antibodies Directed Against Virion Proteins

Overview

Journal J Gen Virol

Specialty Microbiology

Date 1986 Jan 1

PMID 2418148

Citations 62

Authors

H Laude

J M Chapsal

J Gelfi

S Labiau

J Grosclaude

Affiliations

Soon will be listed here.

Abstract

Thirty-two hybridoma cell lines producing monoclonal antibodies (MAbs) against the three major structural proteins of transmissible gastroenteritis virus (TGEV) have been isolated. Radioimmunoprecipitation of intracellular viral polypeptides showed that 17 hybridomas recognized both the peplomer protein [E2, 220 X 10(3) mol. wt. (220K)] and a lower mol. wt. species (E'2, 175K), which was characterized as a precursor of E2. Six MAbs selectively immunoprecipitated the E'2 protein. Four hybridomas were directed against the low mol. wt. envelope protein (E1, 29K), and three against the nucleoprotein (N, 47K). All major neutralization-mediating determinants were found to be carried by the peplomers. Several anti-E2 MAbs displayed an intrinsic neutralizing activity close to that of the most potent anti-TGEV polyclonal reagents tested (including ascitic fluid of feline infectious peritonitis virus-infected cats). None of the anti-E'2 MAbs induced significant neutralization, although this protein might be incorporated to some extent into the virions. Immunofluorescence patterns obtained with MAbs directed against either the envelope glycoproteins or the nucleocapsid revealed distinctly different distributions of these antigens within the cells. Comparison of nine TGEV strains using our panel of MAbs confirmed their close antigenic relationship, but revealed the occurrence of distinct antigenic differences.

Citing Articles

COVID-19 vaccine: where are we now and where should we go?.

Soleimanpour S, Yaghoubi A Expert Rev Vaccines. 2021; 20(1):23-44.

PMID: 33435774 PMC: 7898300. DOI: 10.1080/14760584.2021.1875824.

Étude comparée de trois souches du coronavirus de la gastroentérite transmissible: Conditions de la réplicationvirale et de la synthèse des antigènes structuraux.

Nguyen T, Bernard S, Bottreau E, Lantier I, Aynaud J Ann Inst Pasteur Virol. 2020; 138(3):315-330.

PMID: 32288186 PMC: 7135054. DOI: 10.1016/S0769-2617(87)80018-7.

Inhibition of transmissible gastroenteritis coronavirus (TGEV) multiplication by non-immune lymphocytes.

Charley B, Laude H, La Bonnardiere C Ann Inst Pasteur Virol. 2020; 138(2):183-194.

PMID: 32288183 PMC: 7134748. DOI: 10.1016/S0769-2617(87)80003-5.

Prophylactic and therapeutic effects of egg yolk immunoglobulin against porcine transmissible gastroenteritis virus in piglets.

Zuo Y, Fan J, Fan H, Li T, Zhang X Front Agric China. 2020; 3(1):104-108.

PMID: 32214986 PMC: 7088736. DOI: 10.1007/s11703-008-0080-9.

Evolution, antigenicity and pathogenicity of global porcine epidemic diarrhea virus strains.

Lin C, Saif L, Marthaler D, Wang Q Virus Res. 2016; 226:20-39.

PMID: 27288724 PMC: 7111424. DOI: 10.1016/j.virusres.2016.05.023.