The p15gag and p12gag regions are both necessary for the pathogenicity of the murine AIDS virus

Yoshinao Kubo; Kazuhiro Kakimi; Kyoko Higo; Ling Wang; Hirohiko Kobayashi; Kagemasa Kuribayashi; Toru Masuda; Toshiyasu Hirama; Akinori Ishimoto

The p15^gag and p12^gag regions are both necessary for the pathogenicity of the murine AIDS virus

Yoshinao Kubo, Kazuhiro Kakimi, Kyoko Higo, Ling Wang, Hirohiko Kobayashi, Kagemasa Kuribayashi, Toru Masuda, Toshiyasu Hirama, Akinori Ishimoto

研究成果: ジャーナルへの寄稿 › 学術論文 › 査読

13 被引用数 (Scopus)

抄録

The defective marine AIDS (MAIDS) virus has unique sequences in its p15^gag and p12^gag regions. To clarify whether these sequences are responsible for the development of MAIDS, we constructed recombinant viruses by replacing various regions of the gag gene of the nonpathogenic replication-competent LP-BM5 ecotropic virus with those of the MAIDS virus. Recombinants containing both unique sequences of the MAIDS virus were replication defective and induced MAIDS. However, a recombinant containing either the p15^gag or p12^gag region of the MAIDS virus was also replication defective but nonpathogenic in mice. A recombinant virus containing only the p30^gag region of the MAIDS virus was replication competent and nonpathogenic. These results indicate that the p15^gag and p12^gag regions of the MAIDS virus do not function like those of replication-competent viruses and that both of the unique sequences in the p15^gag and p12^gag regions are required to develop MAIDS.

本文言語	英語
ページ（範囲）	5532-5537
ページ数	6
ジャーナル	Journal of Virology
巻	68
号	9
出版ステータス	出版済み - 09-1994
外部発表	はい

All Science Journal Classification (ASJC) codes

微生物学
免疫学
昆虫科学
ウイルス学

UN SDG

この成果は、次の持続可能な開発目標に貢献しています

他のファイルとリンク

引用スタイル

@article{0d1143166ac2421897fa76a3e761bcc1,

title = "The p15gag and p12gag regions are both necessary for the pathogenicity of the murine AIDS virus",

abstract = "The defective marine AIDS (MAIDS) virus has unique sequences in its p15gag and p12gag regions. To clarify whether these sequences are responsible for the development of MAIDS, we constructed recombinant viruses by replacing various regions of the gag gene of the nonpathogenic replication-competent LP-BM5 ecotropic virus with those of the MAIDS virus. Recombinants containing both unique sequences of the MAIDS virus were replication defective and induced MAIDS. However, a recombinant containing either the p15gag or p12gag region of the MAIDS virus was also replication defective but nonpathogenic in mice. A recombinant virus containing only the p30gag region of the MAIDS virus was replication competent and nonpathogenic. These results indicate that the p15gag and p12gag regions of the MAIDS virus do not function like those of replication-competent viruses and that both of the unique sequences in the p15gag and p12gag regions are required to develop MAIDS.",

author = "Yoshinao Kubo and Kazuhiro Kakimi and Kyoko Higo and Ling Wang and Hirohiko Kobayashi and Kagemasa Kuribayashi and Toru Masuda and Toshiyasu Hirama and Akinori Ishimoto",

year = "1994",

month = sep,

language = "English",

volume = "68",

pages = "5532--5537",

journal = "Journal of Virology",

issn = "0022-538X",

publisher = "American Society for Microbiology",

number = "9",

}

TY - JOUR

T1 - The p15gag and p12gag regions are both necessary for the pathogenicity of the murine AIDS virus

AU - Kubo, Yoshinao

AU - Kakimi, Kazuhiro

AU - Higo, Kyoko

AU - Wang, Ling

AU - Kobayashi, Hirohiko

AU - Kuribayashi, Kagemasa

AU - Masuda, Toru

AU - Hirama, Toshiyasu

AU - Ishimoto, Akinori

PY - 1994/9

Y1 - 1994/9

N2 - The defective marine AIDS (MAIDS) virus has unique sequences in its p15gag and p12gag regions. To clarify whether these sequences are responsible for the development of MAIDS, we constructed recombinant viruses by replacing various regions of the gag gene of the nonpathogenic replication-competent LP-BM5 ecotropic virus with those of the MAIDS virus. Recombinants containing both unique sequences of the MAIDS virus were replication defective and induced MAIDS. However, a recombinant containing either the p15gag or p12gag region of the MAIDS virus was also replication defective but nonpathogenic in mice. A recombinant virus containing only the p30gag region of the MAIDS virus was replication competent and nonpathogenic. These results indicate that the p15gag and p12gag regions of the MAIDS virus do not function like those of replication-competent viruses and that both of the unique sequences in the p15gag and p12gag regions are required to develop MAIDS.

AB - The defective marine AIDS (MAIDS) virus has unique sequences in its p15gag and p12gag regions. To clarify whether these sequences are responsible for the development of MAIDS, we constructed recombinant viruses by replacing various regions of the gag gene of the nonpathogenic replication-competent LP-BM5 ecotropic virus with those of the MAIDS virus. Recombinants containing both unique sequences of the MAIDS virus were replication defective and induced MAIDS. However, a recombinant containing either the p15gag or p12gag region of the MAIDS virus was also replication defective but nonpathogenic in mice. A recombinant virus containing only the p30gag region of the MAIDS virus was replication competent and nonpathogenic. These results indicate that the p15gag and p12gag regions of the MAIDS virus do not function like those of replication-competent viruses and that both of the unique sequences in the p15gag and p12gag regions are required to develop MAIDS.

UR - http://www.scopus.com/inward/record.url?scp=0028169912&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=0028169912&partnerID=8YFLogxK

M3 - Article

C2 - 8057435

AN - SCOPUS:0028169912

SN - 0022-538X

VL - 68

SP - 5532

EP - 5537

JO - Journal of Virology

JF - Journal of Virology

IS - 9

ER -