Sequence analysis of the membrane protein gene of human coronavirus 229E

Patricia Jouvenne; Christopher D. Richardson; Steven S. Schreiber; Michael M.C. Lai; Pierre J. Talbot

doi:10.1016/0042-6822(90)90115-8

Sequence analysis of the membrane protein gene of human coronavirus 229E

Patricia Jouvenne, Christopher D. Richardson, Steven S. Schreiber, Michael M.C. Lai, Pierre J. Talbot

Résultat de recherche: Article › examen par les pairs

11 Citations (Scopus)

Résumé

Human coronaviruses (HCV) are ubiquitous pathogens which cause respiratory, gastrointestinal, and possibly neurological disorders. To better understand the molecular biology of the prototype HCV-229E strain, the complete nucleotide sequence of the membrane protein (M) gene was determined from cloned cDNA. The open reading frame is preceded by a consensus transcriptional initiation sequence UCUAAACU, identical to the one found upstream of the N gene. The M gene encodes a 225-amino acid polypeptide with a molecular weight (MW) of 25,822, slightly higher than the apparent MW of 19,000-22,000 observed for the unprocessed M protein obtained after in vitro translation and immunoprecipitation. The M amino acid sequence presents a significant degree of homology (38%) with its counterpart of transmissible gastroenteritis coronavirus (TGEV). The M protein of HCV-229E is highly hydrophobic and its hydropathicity profile shows a transmembranous region composed of three major hydrophobic domains characteristic of a typical coronavirus M protein. About 10% (20 amino acids) of the HCV-229E M protein constitutes a hydrophilic and probably external portion. One N-glycosylation and three potential O-glycosylation sites are found in this exposed domain.

Langue d'origine	English
Pages (de-à)	608-612
Nombre de pages	5
Journal	Virology
Volume	174
Numéro de publication	2
DOI	https://doi.org/10.1016/0042-6822(90)90115-8
Statut de publication	Published - févr. 1990
Publié à l'externe	Oui

Note bibliographique

Funding Information:
We thank Francois Fossiez for helpful discussions and Lucie Sum-merside for typing the manuscript . This work was supported by Grant MT-9203 from the Medical Research Council of Canada to P . 1 . Talbot, and U .S . Public Health Services Research Grant NS18146 to M. M. C. Lai. P. J. Talbot is also the recipient of a University Research Scholarship from the Natural Sciences and Engineering Research Council of Canada . P . Jouvenne acknowledges a studentship support from the Fonds de la recherche en Same du Quebec . S . S . Schreiber was supported by a postdoctoral training fellowship from the U .S . National Institutes of Health Grant NS07149 .

ASJC Scopus Subject Areas

Virology

Accès au document

10.1016/0042-6822(90)90115-8

Autres fichiers et liens

Citer

@article{542115834d3f488ebb9178172d295263,

title = "Sequence analysis of the membrane protein gene of human coronavirus 229E",

abstract = "Human coronaviruses (HCV) are ubiquitous pathogens which cause respiratory, gastrointestinal, and possibly neurological disorders. To better understand the molecular biology of the prototype HCV-229E strain, the complete nucleotide sequence of the membrane protein (M) gene was determined from cloned cDNA. The open reading frame is preceded by a consensus transcriptional initiation sequence UCUAAACU, identical to the one found upstream of the N gene. The M gene encodes a 225-amino acid polypeptide with a molecular weight (MW) of 25,822, slightly higher than the apparent MW of 19,000-22,000 observed for the unprocessed M protein obtained after in vitro translation and immunoprecipitation. The M amino acid sequence presents a significant degree of homology (38%) with its counterpart of transmissible gastroenteritis coronavirus (TGEV). The M protein of HCV-229E is highly hydrophobic and its hydropathicity profile shows a transmembranous region composed of three major hydrophobic domains characteristic of a typical coronavirus M protein. About 10% (20 amino acids) of the HCV-229E M protein constitutes a hydrophilic and probably external portion. One N-glycosylation and three potential O-glycosylation sites are found in this exposed domain.",

author = "Patricia Jouvenne and Richardson, {Christopher D.} and Schreiber, {Steven S.} and Lai, {Michael M.C.} and Talbot, {Pierre J.}",

note = "Funding Information: We thank Francois Fossiez for helpful discussions and Lucie Sum-merside for typing the manuscript . This work was supported by Grant MT-9203 from the Medical Research Council of Canada to P . 1 . Talbot, and U .S . Public Health Services Research Grant NS18146 to M. M. C. Lai. P. J. Talbot is also the recipient of a University Research Scholarship from the Natural Sciences and Engineering Research Council of Canada . P . Jouvenne acknowledges a studentship support from the Fonds de la recherche en Same du Quebec . S . S . Schreiber was supported by a postdoctoral training fellowship from the U .S . National Institutes of Health Grant NS07149 .",

year = "1990",

month = feb,

doi = "10.1016/0042-6822(90)90115-8",

language = "English",

volume = "174",

pages = "608--612",

journal = "Virology",

issn = "0042-6822",

publisher = "Academic Press Inc.",

number = "2",

}

TY - JOUR

T1 - Sequence analysis of the membrane protein gene of human coronavirus 229E

AU - Jouvenne, Patricia

AU - Richardson, Christopher D.

AU - Schreiber, Steven S.

AU - Lai, Michael M.C.

AU - Talbot, Pierre J.

N1 - Funding Information: We thank Francois Fossiez for helpful discussions and Lucie Sum-merside for typing the manuscript . This work was supported by Grant MT-9203 from the Medical Research Council of Canada to P . 1 . Talbot, and U .S . Public Health Services Research Grant NS18146 to M. M. C. Lai. P. J. Talbot is also the recipient of a University Research Scholarship from the Natural Sciences and Engineering Research Council of Canada . P . Jouvenne acknowledges a studentship support from the Fonds de la recherche en Same du Quebec . S . S . Schreiber was supported by a postdoctoral training fellowship from the U .S . National Institutes of Health Grant NS07149 .

PY - 1990/2

Y1 - 1990/2

N2 - Human coronaviruses (HCV) are ubiquitous pathogens which cause respiratory, gastrointestinal, and possibly neurological disorders. To better understand the molecular biology of the prototype HCV-229E strain, the complete nucleotide sequence of the membrane protein (M) gene was determined from cloned cDNA. The open reading frame is preceded by a consensus transcriptional initiation sequence UCUAAACU, identical to the one found upstream of the N gene. The M gene encodes a 225-amino acid polypeptide with a molecular weight (MW) of 25,822, slightly higher than the apparent MW of 19,000-22,000 observed for the unprocessed M protein obtained after in vitro translation and immunoprecipitation. The M amino acid sequence presents a significant degree of homology (38%) with its counterpart of transmissible gastroenteritis coronavirus (TGEV). The M protein of HCV-229E is highly hydrophobic and its hydropathicity profile shows a transmembranous region composed of three major hydrophobic domains characteristic of a typical coronavirus M protein. About 10% (20 amino acids) of the HCV-229E M protein constitutes a hydrophilic and probably external portion. One N-glycosylation and three potential O-glycosylation sites are found in this exposed domain.

AB - Human coronaviruses (HCV) are ubiquitous pathogens which cause respiratory, gastrointestinal, and possibly neurological disorders. To better understand the molecular biology of the prototype HCV-229E strain, the complete nucleotide sequence of the membrane protein (M) gene was determined from cloned cDNA. The open reading frame is preceded by a consensus transcriptional initiation sequence UCUAAACU, identical to the one found upstream of the N gene. The M gene encodes a 225-amino acid polypeptide with a molecular weight (MW) of 25,822, slightly higher than the apparent MW of 19,000-22,000 observed for the unprocessed M protein obtained after in vitro translation and immunoprecipitation. The M amino acid sequence presents a significant degree of homology (38%) with its counterpart of transmissible gastroenteritis coronavirus (TGEV). The M protein of HCV-229E is highly hydrophobic and its hydropathicity profile shows a transmembranous region composed of three major hydrophobic domains characteristic of a typical coronavirus M protein. About 10% (20 amino acids) of the HCV-229E M protein constitutes a hydrophilic and probably external portion. One N-glycosylation and three potential O-glycosylation sites are found in this exposed domain.

UR - http://www.scopus.com/inward/record.url?scp=0025022501&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=0025022501&partnerID=8YFLogxK

U2 - 10.1016/0042-6822(90)90115-8

DO - 10.1016/0042-6822(90)90115-8

M3 - Article

C2 - 2305554

AN - SCOPUS:0025022501

SN - 0042-6822

VL - 174

SP - 608

EP - 612

JO - Virology

JF - Virology

IS - 2

ER -

Sequence analysis of the membrane protein gene of human coronavirus 229E

Résumé

Note bibliographique

ASJC Scopus Subject Areas

Accès au document

Autres fichiers et liens

Empreinte numérique

Citer