Chemical Library Screens Targeting an HIV-1 Accessory Factor/Host Cell Kinase Complex Identify Novel Antiretroviral Compounds

Emert-Sedlak, Lori A.; Kodama, Toshiaki; Lerner, Edwina C.; Dai, Weixiang; Foster, Caleb; Day, Billy W.; Lazo, John S.; Smithgall, Thomas E.

doi:10.1021/cb900195c

Cited by 59 publications

(118 citation statements)

References 38 publications

Supporting

Mentioning

112

Contrasting

Order By: Relevance

“…Recent work has established that selective inhibitors of Nef-induced SFK activation block Nef-dependent HIV infectivity and replication in cell culture (21)(22)(23). These studies support the idea that interaction of Nef with SH3-containing kinases and other proteins is a common event in HIV-infected cells that generates downstream signals essential for viral pathogenesis.…”

mentioning

confidence: 63%

The Accessory Factor Nef Links HIV-1 to Tec/Btk Kinases in an Src Homology 3 Domain-dependent Manner

Tarafdar

Poe

Smithgall

2014

Journal of Biological Chemistry

Self Cite

View full text Add to dashboard Cite

mentioning

confidence: 63%

The Accessory Factor Nef Links HIV-1 to Tec/Btk Kinases in an Src Homology 3 Domain-dependent Manner

Tarafdar

Poe

Smithgall

2014

Journal of Biological Chemistry

Self Cite

View full text Add to dashboard Cite

“…The resulting binding constants are summarized below the graphs. Nef⅐Hck complex, which is essential for Nef function and represents a druggable target for HIV-1 (14,16,17,21). Finally, the Nef dimer that results from Hck SH3-SH2 binding allows for surface display of Nef residue Asp-123, which plays a critical role in multiple Nef functions including CD4 and MHC-I down-regulation (32,43,61) as well as enhancement of viral replication (43).…”

Section: Sh3 Glu-93 Is Required For High Affinity Binding Of Nef Tomentioning

confidence: 99%

Interaction with the Src Homology (SH3-SH2) Region of the Src-family Kinase Hck Structures the HIV-1 Nef Dimer for Kinase Activation and Effector Recruitment

Alvarado

Tarafdar

Yeh

et al. 2014

Journal of Biological Chemistry

Self Cite

View full text Add to dashboard Cite

“…VSL12 mass and purity were verified by mass spectrometry. In vitro kinase assays were performed using the Tyr-2 FRET peptide substrate and the Z'-Lyte TM assay (Invitrogen) as described previously (14,17).…”

Section: Expression and Purification Of Recombinant Sfks And In Vitromentioning

confidence: 99%

Crystal Structure of the Src Family Kinase Hck SH3-SH2 Linker Regulatory Region Supports an SH3-dominant Activation Mechanism

Alvarado

Betts

Moroco

et al. 2010

Journal of Biological Chemistry

Self Cite

View full text Add to dashboard Cite

Most mammalian cell types depend on multiple Src family kinases (SFKs) to regulate diverse signaling pathways. Strict control of SFK activity is essential for normal cellular function, and loss of kinase regulation contributes to several forms of cancer and other diseases. Previous x-ray crystal structures of the SFKs c-Src and Hck revealed that intramolecular association of their Src homology (SH) 3 domains and SH2 kinase linker regions has a key role in down-regulation of kinase activity. However, the amino acid sequence of the Hck linker represents a suboptimal ligand for the isolated SH3 domain, suggesting that it may form the polyproline type II helical conformation required for SH3 docking only in the context of the intact structure. To test this hypothesis directly, we determined the crystal structure of a truncated Hck protein consisting of the SH2 and SH3 domains plus the linker. Despite the absence of the kinase domain, the structures and relative orientations of the SH2 and SH3 domains in this shorter protein were very similar to those observed in near full-length, down-regulated Hck. However, the SH2 kinase linker adopted a modified topology and failed to engage the SH3 domain. This new structure supports the idea that these noncatalytic regions work together as a "conformational switch" that modulates kinase activity in a manner unique to the SH3 domain and linker topologies present in the intact Hck protein. Our results also provide fresh structural insight into the facile induction of Hck activity by HIV-1 Nef and other Hck SH3 domain binding proteins and implicate the existence of innate conformational states unique to individual Src family members that "fine-tune" their sensitivities to activation by SH3-based ligands.

show abstract

Chemical Library Screens Targeting an HIV-1 Accessory Factor/Host Cell Kinase Complex Identify Novel Antiretroviral Compounds

Cited by 59 publications

References 38 publications

The Accessory Factor Nef Links HIV-1 to Tec/Btk Kinases in an Src Homology 3 Domain-dependent Manner

The Accessory Factor Nef Links HIV-1 to Tec/Btk Kinases in an Src Homology 3 Domain-dependent Manner

Interaction with the Src Homology (SH3-SH2) Region of the Src-family Kinase Hck Structures the HIV-1 Nef Dimer for Kinase Activation and Effector Recruitment

Crystal Structure of the Src Family Kinase Hck SH3-SH2 Linker Regulatory Region Supports an SH3-dominant Activation Mechanism

Contact Info

Product

Resources

About