Drugs that stimulate internalization of CCR5 may effectively inhibit HIV infection, both by decreasing cell surface expression of CCR5 and by stabilizing receptor conformations that inhibit fusion of virus that binds to drug-occupied receptor.AcknowledgmentsThe HIV-1C env construct pTHr.gp150CT [31] was a generous gift from Carolyn Williamson (University of Cape Town). The HIV-1 tat, HIV-1 rev and the pHIV-1LTR-Luc reporter construct were generously provided byConstitutively Active CCR5 Receptor ConformationsSteven Jenkinson, GlaxoSmithKline. The following cell lines were obtained from the AIDS Research and Reference Reagent Program, Division of AIDS, NIAID, NIH: Human osteosarcoma cells stably expressing CD4 (HOS-CD4.pBABE-puro) or CD4 and CCR5 (HOS-CD4-CCR5) from Dr Nathaniel Landau [33].Author ContributionsConceived and designed the experiments: AdV CAF. Performed the experiments: AdV CAF. Analyzed the data: AdV CAF. Contributed reagents/materials/analysis tools: ATF MCC. 17460038 Wrote the paper: AdV MTM CAF.
Eukaryotic cells require endocytosis for uptake of extra-cellular substances and internalization of plasma membrane proteins for GSK-J4 site transport to endosomes [1]. Endocytosis regulates and is involved in many important processes, including several signaling pathways [2,3,4]. Plants require endocytosis for important processes including development [5] and defense against microorganisms [6,7]. Studies conducted in plant systems have elucidated possible functionalities of plant endocytic compartments and the flow of endocytosed material throughout plant cells [7,8,9,10,11,12,13,14]. Endocytosis depends on a large number of protein-protein interactions mediated by specific modules. One such module is the EH (Eps15 homology) GSK3326595 chemical information domain first identified in Eps15 [15,16]. The EH domain structure generally consists of two EF-hands and a helix-loop-helix structure that binds calcium (or a pseudo EFhand), connected by an anti-parallel beta-sheet [17,18,19]. Many EH-containing proteins were identified in different species, among them EHD1-4 (EH domain containing proteins), Eps15 and Intersectin 1? [20,21,22,23]. Four EHD orthologs are known in vertebrates [24] and two in plants [25]. All mammalian EHDs share a similar structure: An Nterminal domain with a nucleotide binding motif (P-loop), DxxG and NKxD, a central coiled coil region and a C-terminal EH domain containing an EF Ca2+ binding motif. C-terminal EH domain containing proteins are regulators of endocytic trafficking,and have been shown to associate with Rab protein effectors [24,26]. Despite their high homology (70?0 ) the mammalian EHDs differ in the transport steps which they regulate [20,27,28,29]. Mammalian EHD1 was shown to regulate the recycling of many receptors [30], endocytosed via both clathrin [31] and non clathrin pathways [32,33]. Based on the knowledge to date, EHD1 is involved primarily in recycling from the endocytic recycling compartment (ERC) to the plasma membrane. In addition, evidence suggests that EHD1 is involved not only in recycling to the plasma membrane, but also in transport of receptors from the early endosome to the ERC [26,34], as well as in retrograde transport from endosomes to golgi [35]. EHD3, which shares the highest level of homology with EHD1 amongst the mammalian EHD proteins, is also involved in endosome to golgi transport and appears to be required for maintenance of golgi morphology and function [36]. We previously reported the isolation and characterization.Drugs that stimulate internalization of CCR5 may effectively inhibit HIV infection, both by decreasing cell surface expression of CCR5 and by stabilizing receptor conformations that inhibit fusion of virus that binds to drug-occupied receptor.AcknowledgmentsThe HIV-1C env construct pTHr.gp150CT [31] was a generous gift from Carolyn Williamson (University of Cape Town). The HIV-1 tat, HIV-1 rev and the pHIV-1LTR-Luc reporter construct were generously provided byConstitutively Active CCR5 Receptor ConformationsSteven Jenkinson, GlaxoSmithKline. The following cell lines were obtained from the AIDS Research and Reference Reagent Program, Division of AIDS, NIAID, NIH: Human osteosarcoma cells stably expressing CD4 (HOS-CD4.pBABE-puro) or CD4 and CCR5 (HOS-CD4-CCR5) from Dr Nathaniel Landau [33].Author ContributionsConceived and designed the experiments: AdV CAF. Performed the experiments: AdV CAF. Analyzed the data: AdV CAF. Contributed reagents/materials/analysis tools: ATF MCC. 17460038 Wrote the paper: AdV MTM CAF.
Eukaryotic cells require endocytosis for uptake of extra-cellular substances and internalization of plasma membrane proteins for transport to endosomes [1]. Endocytosis regulates and is involved in many important processes, including several signaling pathways [2,3,4]. Plants require endocytosis for important processes including development [5] and defense against microorganisms [6,7]. Studies conducted in plant systems have elucidated possible functionalities of plant endocytic compartments and the flow of endocytosed material throughout plant cells [7,8,9,10,11,12,13,14]. Endocytosis depends on a large number of protein-protein interactions mediated by specific modules. One such module is the EH (Eps15 homology) domain first identified in Eps15 [15,16]. The EH domain structure generally consists of two EF-hands and a helix-loop-helix structure that binds calcium (or a pseudo EFhand), connected by an anti-parallel beta-sheet [17,18,19]. Many EH-containing proteins were identified in different species, among them EHD1-4 (EH domain containing proteins), Eps15 and Intersectin 1? [20,21,22,23]. Four EHD orthologs are known in vertebrates [24] and two in plants [25]. All mammalian EHDs share a similar structure: An Nterminal domain with a nucleotide binding motif (P-loop), DxxG and NKxD, a central coiled coil region and a C-terminal EH domain containing an EF Ca2+ binding motif. C-terminal EH domain containing proteins are regulators of endocytic trafficking,and have been shown to associate with Rab protein effectors [24,26]. Despite their high homology (70?0 ) the mammalian EHDs differ in the transport steps which they regulate [20,27,28,29]. Mammalian EHD1 was shown to regulate the recycling of many receptors [30], endocytosed via both clathrin [31] and non clathrin pathways [32,33]. Based on the knowledge to date, EHD1 is involved primarily in recycling from the endocytic recycling compartment (ERC) to the plasma membrane. In addition, evidence suggests that EHD1 is involved not only in recycling to the plasma membrane, but also in transport of receptors from the early endosome to the ERC [26,34], as well as in retrograde transport from endosomes to golgi [35]. EHD3, which shares the highest level of homology with EHD1 amongst the mammalian EHD proteins, is also involved in endosome to golgi transport and appears to be required for maintenance of golgi morphology and function [36]. We previously reported the isolation and characterization.
