Constrained use of CCR5 on CD4+ lymphocytes by R5X4 HIV-1: Efficiency of Env-CCR5 interactions and low CCR5 expression determine a range of restricted CCR5-mediated entry

Lamorris M. Loftin; Martha F. Kienzle; Yanjie Yi; Benhur Lee; Fang Hua Lee; Lachlan Gray; Paul R. Gorry; Ronald G. Collman

doi:10.1016/j.virol.2010.03.009

Constrained use of CCR5 on CD4+ lymphocytes by R5X4 HIV-1: Efficiency of Env-CCR5 interactions and low CCR5 expression determine a range of restricted CCR5-mediated entry

Lamorris M. Loftin
, Martha F. Kienzle
, Yanjie Yi
, Benhur Lee
, Fang Hua Lee
, Lachlan Gray
, Paul R. Gorry
, Ronald G. Collman

Research output: Contribution to journal › Article › peer-review

12 Scopus citations

Abstract

R5X4 HIV-1 has impaired utilization of CCR5 on primary CD4+ lymphocytes but the mechanisms responsible are not well defined. Using a panel of diverse R5X4 Envs we identified a spectrum of CCR5 use on CD4+ lymphocytes. Greater lymphocyte CCR5 use correlated with relative resistance to CCR5 mAbs and small molecule antagonists. Increasing CCR5 expression on lymphocytes increased the proportion of entry mediated by CCR5 for all R5X4 isolates except 89.6. In cell lines with regulated CCR5 expression, strains with greater lymphocyte CCR5 use better exploited limiting levels of CCR5. Introduction of an R306S mutation in the 89.6 V3 domain enhanced its utilization of CCR5 at low levels and switched its preference to CCR5 for lymphocyte entry. Thus, the degree to which R5X4 HIV-1 use primary lymphocyte CCR5 is determined by low CCR5 expression coupled with variations in the efficiency of Env-CCR5 interactions, which is in part governed by V3 sequences.

Original language	English
Pages (from-to)	135-148
Number of pages	14
Journal	Virology
Volume	402
Issue number	1
DOIs	https://doi.org/10.1016/j.virol.2010.03.009
State	Published - Jun 2010
Externally published	Yes

Keywords

CCR5
CD4+ lymphocytes
Coreceptor use
HIV-1 tropism
R5X4 HIV-1
Viral entry

Access to Document

10.1016/j.virol.2010.03.009

Cite this

@article{54fc4b133e9042c7a8f8ecea98eea627,

title = "Constrained use of CCR5 on CD4+ lymphocytes by R5X4 HIV-1: Efficiency of Env-CCR5 interactions and low CCR5 expression determine a range of restricted CCR5-mediated entry",

abstract = "R5X4 HIV-1 has impaired utilization of CCR5 on primary CD4+ lymphocytes but the mechanisms responsible are not well defined. Using a panel of diverse R5X4 Envs we identified a spectrum of CCR5 use on CD4+ lymphocytes. Greater lymphocyte CCR5 use correlated with relative resistance to CCR5 mAbs and small molecule antagonists. Increasing CCR5 expression on lymphocytes increased the proportion of entry mediated by CCR5 for all R5X4 isolates except 89.6. In cell lines with regulated CCR5 expression, strains with greater lymphocyte CCR5 use better exploited limiting levels of CCR5. Introduction of an R306S mutation in the 89.6 V3 domain enhanced its utilization of CCR5 at low levels and switched its preference to CCR5 for lymphocyte entry. Thus, the degree to which R5X4 HIV-1 use primary lymphocyte CCR5 is determined by low CCR5 expression coupled with variations in the efficiency of Env-CCR5 interactions, which is in part governed by V3 sequences.",

keywords = "CCR5, CD4+ lymphocytes, Coreceptor use, HIV-1 tropism, R5X4 HIV-1, Viral entry",

author = "Loftin, \{Lamorris M.\} and Kienzle, \{Martha F.\} and Yanjie Yi and Benhur Lee and Lee, \{Fang Hua\} and Lachlan Gray and Gorry, \{Paul R.\} and Collman, \{Ronald G.\}",

note = "Funding Information: We thank M. Mack and M. Betts for the mAbs and M. Miller for M657. We also thank R. Doms, J. Hoxie, L. Su and M. Cho for the HIV-1 Envs. We are grateful to J. Sodroski, P. Corbeau and B. Cullen for the various constructs and vectors. We also acknowledge the valuable support for this work from the Immunology, the Biostatistics and the Viral/Molecular Cores of the Penn Center for AIDS Research. This work was supported by NIH grant R01 AI035502 (R.G.C.). L.L. was supported in part by NIH T32 AI007632 and P.R.G. is the recipient of an Australian National Health and Medical Research Council Level 2 Biomedical Career Development Award.",

year = "2010",

month = jun,

doi = "10.1016/j.virol.2010.03.009",

language = "English",

volume = "402",

pages = "135--148",

journal = "Virology",

issn = "0042-6822",

publisher = "Academic Press Inc.",

number = "1",

}

TY - JOUR

T1 - Constrained use of CCR5 on CD4+ lymphocytes by R5X4 HIV-1

T2 - Efficiency of Env-CCR5 interactions and low CCR5 expression determine a range of restricted CCR5-mediated entry

AU - Loftin, Lamorris M.

AU - Kienzle, Martha F.

AU - Yi, Yanjie

AU - Lee, Benhur

AU - Lee, Fang Hua

AU - Gray, Lachlan

AU - Gorry, Paul R.

AU - Collman, Ronald G.

N1 - Funding Information: We thank M. Mack and M. Betts for the mAbs and M. Miller for M657. We also thank R. Doms, J. Hoxie, L. Su and M. Cho for the HIV-1 Envs. We are grateful to J. Sodroski, P. Corbeau and B. Cullen for the various constructs and vectors. We also acknowledge the valuable support for this work from the Immunology, the Biostatistics and the Viral/Molecular Cores of the Penn Center for AIDS Research. This work was supported by NIH grant R01 AI035502 (R.G.C.). L.L. was supported in part by NIH T32 AI007632 and P.R.G. is the recipient of an Australian National Health and Medical Research Council Level 2 Biomedical Career Development Award.

PY - 2010/6

Y1 - 2010/6

N2 - R5X4 HIV-1 has impaired utilization of CCR5 on primary CD4+ lymphocytes but the mechanisms responsible are not well defined. Using a panel of diverse R5X4 Envs we identified a spectrum of CCR5 use on CD4+ lymphocytes. Greater lymphocyte CCR5 use correlated with relative resistance to CCR5 mAbs and small molecule antagonists. Increasing CCR5 expression on lymphocytes increased the proportion of entry mediated by CCR5 for all R5X4 isolates except 89.6. In cell lines with regulated CCR5 expression, strains with greater lymphocyte CCR5 use better exploited limiting levels of CCR5. Introduction of an R306S mutation in the 89.6 V3 domain enhanced its utilization of CCR5 at low levels and switched its preference to CCR5 for lymphocyte entry. Thus, the degree to which R5X4 HIV-1 use primary lymphocyte CCR5 is determined by low CCR5 expression coupled with variations in the efficiency of Env-CCR5 interactions, which is in part governed by V3 sequences.

AB - R5X4 HIV-1 has impaired utilization of CCR5 on primary CD4+ lymphocytes but the mechanisms responsible are not well defined. Using a panel of diverse R5X4 Envs we identified a spectrum of CCR5 use on CD4+ lymphocytes. Greater lymphocyte CCR5 use correlated with relative resistance to CCR5 mAbs and small molecule antagonists. Increasing CCR5 expression on lymphocytes increased the proportion of entry mediated by CCR5 for all R5X4 isolates except 89.6. In cell lines with regulated CCR5 expression, strains with greater lymphocyte CCR5 use better exploited limiting levels of CCR5. Introduction of an R306S mutation in the 89.6 V3 domain enhanced its utilization of CCR5 at low levels and switched its preference to CCR5 for lymphocyte entry. Thus, the degree to which R5X4 HIV-1 use primary lymphocyte CCR5 is determined by low CCR5 expression coupled with variations in the efficiency of Env-CCR5 interactions, which is in part governed by V3 sequences.

KW - CCR5

KW - CD4+ lymphocytes

KW - Coreceptor use

KW - HIV-1 tropism

KW - R5X4 HIV-1

KW - Viral entry

UR - https://www.scopus.com/pages/publications/77952554637

U2 - 10.1016/j.virol.2010.03.009

DO - 10.1016/j.virol.2010.03.009

M3 - Article

C2 - 20381825

AN - SCOPUS:77952554637

SN - 0042-6822

VL - 402

SP - 135

EP - 148

JO - Virology

JF - Virology

IS - 1

ER -

Constrained use of CCR5 on CD4+ lymphocytes by R5X4 HIV-1: Efficiency of Env-CCR5 interactions and low CCR5 expression determine a range of restricted CCR5-mediated entry

Abstract

Keywords

Access to Document

Fingerprint

Cite this