Inhibitory mechanism of the CXCR4 antagonist t22 against human immunodeficiency virus type 1 infection

被引：88

作者：

Murakami, T

Zhang, TY

Koyanagi, Y

Tanaka, Y

Kim, J

Suzuki, Y

Minoguchi, S

Tamamura, H

Waki, M

Matsumoto, A

Fujii, N

Shida, H

Hoxie, JA

Peiper, SC

Yamamoto, N

机构：

[1] Tokyo Med & Dent Univ, Fac Med, Dept Microbiol & Mol Virol, Bunkyo Ku, Tokyo 1138519, Japan

[2] Univ Ryukyus, Okinawa 9030215, Japan

[3] Kyoto Univ, Inst Virus Res, Kyoto 60601, Japan

[4] Kyoto Univ, Grad Sch Pharmaceut Sci, Kyoto 6068501, Japan

[5] Seikagaku Corp, Tokyo 103, Japan

[6] Kyoto Univ, Fac Med, Dept Med Chem, Sakyo Ku, Kyoto 606, Japan

[7] Univ Louisville, Louisville, KY 40202 USA

[8] Genentech Inc, San Francisco, CA 94080 USA

[9] Univ Penn, Philadelphia, PA 19104 USA

来源：

JOURNAL OF VIROLOGY | 1999年 / 73卷 / 09期

关键词：

D O I：

10.1128/JVI.73.9.7489-7496.1999

中图分类号：

Q93 [微生物学];

学科分类号：

071005 ; 100705 ;

摘要：

We recently reported that a cationic peptide, T22 ([Tyr(5,12), Lys(7)]-polyphemusin II), specifically inhibits human immunodeficiency virus type 1 (HIV-1) infection mediated by CXCR4 (T. Murakami ct al., J. Exp. Med. 186:1389-1393, 1997). Here we demonstrate that T22 effectively inhibits replication of T-tropic HIV-1, including primary isolates, but not of non-T-tropic strains. By using a panel of chimeric viruses between T- and M-tropic HIV-1 strains, viral determinants for T22 susceptibility were mapped to the V3 loop region of gp120. T22 bound to CXCR4 and interfered with stromal-cell-derived factor-1 alpha-CXCR4 interactions in a competitive manner. Blocking of anti-CXCR4 monoclonal antibodies by T22 suggested that the peptide interacts with the N terminus and two of the extracellular loops of CXCR4. Furthermore, the inhibition of cell-cell fusion in cells expressing CXCR4/CXCR2 chimeric receptors suggested that determinants for sensitivity of CXCR4 to T22 include the three extracellular loops of the coreceptor.

引用

页码：7489 / 7496

页数：8

共 74 条

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