Internalization of the human immunodeficiency virus does not require the cytoplasmic domain of CD4

Bedinger, Patricia A.; Moriarty, Ann; Borstel, R. C. von; Donovan, Nancy J.; Steimer, Kathelyn S.; Littman, Dan R.

doi:10.1038/334162a0

Cited by 169 publications

(122 citation statements)

References 29 publications

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“…When alkaline phosphatase is anchored in the same manner it forms tetramers (Hawrylak & Stinson, 1988). The intracellular domain of CD4 is not necessary for HIV entry, since cells transfected with CD4 without the cytoplasmic domain support HIV infection and cells expressing a CD4-CD8 chimera which contains the D1D2 region of CD4 and the hinge, transmembrane and cytoplasmic domains of human CD8 were susceptible to HIV-1 infection (at very low efficiency) (Bedinger et al, 1988). After the completion of this study, Langedijk e t al.…”

Section: Discussionmentioning

confidence: 97%

Analysis of the human immunodeficiency virus type 1 envelope protein interaction with the CD4 host cell receptor

Malvoisin

Wild

1994

Journal of General Virology

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A secreted form of human immunodeficiency virus type 1 (HIV-1) envelope glycoprotein (gpl60s), expressed in HeLa cells from a vaccinia virus recombinant was analysed by velocity-gradient centrifugation and chemical cross-linking. We showed that gpl60s existed predominantly as a dimer, but higher forms corresponding to trimers and tetramers were also found. Soluble CD4 (sCD4) and native CD4 expressed by recombinant vaccinia viruses were analysed by sucrosegradient sedimentation alone or after complexing with gpl60s. The sCD4 sedimented in sucrose gradients as a monomer, whereas after solubilization the native CD4 was in a dimeric state. Both forms of CD4 were able to form complexes when incubated with gpl60s. In the case of the sCD4, the Mr corresponded to a (sCD4) 2-(gpl60s)2 complex, whereas with CD4 the complexes were of a greater order of magnitude. HIV gpl20 was secreted into the medium in a monomeric state, With sCD4 it gave a one-to-one complex, whereas with the native CD4 high M r complexes were formed. The importance of the oligomeric state of the virus-and cell-receptor proteins are discussed regarding their avidities.

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Section: Discussionmentioning

confidence: 97%

Analysis of the human immunodeficiency virus type 1 envelope protein interaction with the CD4 host cell receptor

Malvoisin

Wild

1994

Journal of General Virology

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“…The foxa2 targeting construct (Fig. 6A, which is published as supporting information on the PNAS web site) contains a truncated version of the human CD4 cDNA that lacks most of the intracellular signaling domain (16). GFP-Bry ES cells were electroporated with the foxa2 targeting vector, and appropriately targeted clones were identified by Southern blot analysis (Fig.…”

Section: Resultsmentioning

confidence: 99%

Wnt and TGF-β signaling are required for the induction of an in vitro model of primitive streak formation using embryonic stem cells

Gadue

Huber

Paddison

et al. 2006

Proc. Natl. Acad. Sci. U.S.A.

510

505

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The establishment of the primitive streak and its derivative germ layers, mesoderm and endoderm, are prerequisite steps in the formation of many tissues. To model these developmental stages in vitro, an ES cell line was established that expresses CD4 from the foxa2 locus in addition to GFP from the brachyury locus. A GFP-Bry ؉ population expressing variable levels of CD4-Foxa2 developed upon differentiation of this ES cell line. Analysis of gene-expression patterns and developmental potential revealed that the CD4-Foxa2 hi GFP-Bry ؉ population displays characteristics of the anterior primitive streak, whereas the CD4-Foxa2 lo GFP-Bry ؉ cells resemble the posterior streak. Using this model, we were able to demonstrate that Wnt and TGF-␤͞nodal͞activin signaling simultaneously were required for the generation of the CD4-Foxa2 ؉ GFP-Bry ؉ population. Wnt or low levels of activin-induced a posterior primitive streak population, whereas high levels of activin resulted in an anterior streak fate. Finally, sustained activin signaling was found to stimulate endoderm commitment from the CD4-Foxa2 ؉ GFP-Bry ؉ ES cell population. These findings demonstrate that the early developmental events involved in germ-layer induction in the embryo are recapitulated in the ES cell model and uncover insights into the signaling pathways involved in the establishment of mesoderm and endoderm.gastrulation ͉ mesoderm ͉ endoderm T o be able to fully exploit the potential of embryonic stem (ES) cells in basic biology and regenerative medicine, it is essential to recapitulate the critical lineage induction events of the early embryo in this model system. One of the earliest commitment steps in embryogenesis is the formation of the primary germ layers, mesoderm, endoderm, and ectoderm, the founder populations of all somatic cell types in the body (1). Mesoderm and endoderm are formed during gastrulation, a process that involves the movement of undifferentiated epiblast cells through a structure called the primitive streak (PS). The PS can be subdivided into distinct regions, posterior, middle, and anterior, based on lineage development and gene-expression patterns. With respect to developmental potential, distinct subpopulations of mesoderm are induced in each of the different regions, whereas definitive endoderm forms from the anterior PS of the early-PS and mid-PS stages (2-5). These observations suggest that the different regions of the PS constitute different signaling environments that are responsible for the induction of specific lineages.To address questions regarding early commitment by using the ES cell model, it is essential to be able to track and isolate germ-layer populations from the differentiation cultures. By using an ES cell line with the green fluorescence protein (GFP) targeted to the PS and early mesodermal-specific gene brachyury (6) (GFPBry ES cells), it has been possible to quantify mesoderm induction and isolate and characterize different mesodermal populations (7,8). In addition, brachyury-expressing cells were found ...

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“…Like certain enveloped viruses such as Herpes Simplex virus-1 and Sendai virus, HIV entry was shown to be independent of pH and/or presence of lysosomal enzymes thus suggesting that virus entry into endolysosomal compartments was not required [19][20][21][22][23][24][25][26][27][28][29][30][31]. Studies with CD4 truncation mutations supported this view as mutations that tethered CD4 at the membrane did not impede HIV entry [20,22,23]. Furthermore, HIV Env on the surface of infected cells could induce "fusion from without" with CD4 molecules present on target cells at neutral pH [32] and finally HIV was shown to overcome post-entry block of the actin cortex which can act as a barrier to viruses entering by direct fusion rather than endocytosis [33,34].…”

Section: Entry At Plasma Membrane Vs Endocytosismentioning

confidence: 99%

Resolving the Sites of HIV Entry: Dynamin Networks Hold the Key

Aggarwal¹,

Turville²

2017

J Cell Signal

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HIV/AIDS pandemic continues to represent a major health concern worldwide and novel strategies are being devised to develop a cure for HIV infection. Central to this is a deeper understanding of host-virus interactions especially at the point of virus entry. HIV can enter target cells either by direct fusion with the plasma membrane or via endocytosis. Herein, we will review the evidence for and against either pathway especially in the context of quiescent CD4 T cells, arguably the most important cellular latent reservoir for HIV. The use of complementary approaches such as single molecule imaging, molecular techniques and small molecule inhibitors have greatly added to our understanding of HIV fusion sites. Cellular GTPase dynamin has emerged as a key player in the process given its ability to modulate HIV infection during virus entry and at later stages of virus replication cycle. These new insights into HIV fusion process in physiologically relevant target cells may in turn be leveraged to advance not only HIV cure efforts, but also immunotherapy.

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Internalization of the human immunodeficiency virus does not require the cytoplasmic domain of CD4

Cited by 169 publications

References 29 publications

Analysis of the human immunodeficiency virus type 1 envelope protein interaction with the CD4 host cell receptor

Analysis of the human immunodeficiency virus type 1 envelope protein interaction with the CD4 host cell receptor

Wnt and TGF-β signaling are required for the induction of an in vitro model of primitive streak formation using embryonic stem cells

Resolving the Sites of HIV Entry: Dynamin Networks Hold the Key

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