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Dive into the research topics where Waleed Danho is active.

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Featured researches published by Waleed Danho.


Journal of Biological Chemistry | 1996

Interaction of Phosphorylated FcϵRIγ Immunoglobulin Receptor Tyrosine Activation Motif-based Peptides with Dual and Single SH2 Domains of p72syk ASSESSMENT OF BINDING PARAMETERS AND REAL TIME BINDING KINETICS

Ting Chen; Barbara Repetto; Richard Anthony Chizzonite; Christine E. Pullar; Charles Burghardt; Elizabeth Dharm; Zhicheng Zhao; Robert Carroll; Perla Nunes; Mitali Basu; Waleed Danho; Mike Visnick; Jarema Peter Kochan; David S. Waugh; Alasdair M. Gilfillan

To examine the characteristics of the interaction of the FcεRIγ ITAM with the SH2 domains of p72syk, the binding of an 125I-labeled dual phosphorylated FcεRIγ ITAM-based peptide to the p72syk SH2 domains was monitored utilizing a novel scintillation proximity based assay. The Kd for this interaction, determined from the saturation binding isotherm, was 1.4 nM. This high affinity binding was reflected in the rapid rate of association for the peptide binding to the SH2 domains. Competition studies utilizing a soluble C-terminal SH2 domain knockout and N-terminal SH2 domain knockouts revealed that both domains contribute cooperatively to the high affinity binding. Unlabeled dual phosphorylated peptide competed with the 125I-labeled peptide for binding to the dual p72syk SH2 domains with an IC50 value of 4.8 nM. Monophosphorylated 24-mer FcεRIγ ITAM peptides, and phosphotyrosine also competed for binding, but with substantially higher IC50 values. This, and other data discussed, suggest that high affinity binding requires both tyrosine residues to be phosphorylated and that the preferred binding orientation of the ITAM is such that the N-terminal phosphotyrosine occupies the C-terminal SH2 domain and the C-terminal phosphotyrosine occupies the N-terminal SH2 domain.


Journal of Biological Chemistry | 1998

The N-terminal Domain of RGS4 Confers Receptor-selective Inhibition of G Protein Signaling

Weizhang Zeng; Xin Xu; Serguei Popov; Suchetana Mukhopadhyay; Peter Chidiac; Joseph Swistok; Waleed Danho; Keith A. Yagaloff; Stewart L. Fisher; Elliott M. Ross; Shmuel Muallem; Thomas M. Wilkie


Archive | 2001

Selective cyclic peptides with melanocortin-4 receptor (MC4-R) agonist activity

Li Chen; Adrian Wai-Hing Cheung; Xin-Jie Chu; Waleed Danho; Joseph Swistok; Yao Wang; Keith A. Yagaloff


Journal of Medicinal Chemistry | 1991

Carboxylic acids and tetrazoles as isosteric replacements for sulfate in cholecystokinin analogues.

Jefferson Wright Tilley; Waleed Danho; Kathleen Lovey; Rolf Wagner; Joseph Swistok; Raymond C. Makofske; Joseph Michalewsky; Joseph Triscari; David L. Nelson; Sally Weatherford


Archive | 1989

Cholecystokinin analogs for controlling appetite

Waleed Danho; Vincent S. Madison; Joseph Triscari


Journal of Medicinal Chemistry | 1992

Analogs of Ac-CCK-7 incorporating dipeptide mimics in place of Met28-Gly29

Jefferson Wright Tilley; Waleed Danho; Shiuey Sj; Kulesha I; Joseph Swistok; Raymond C. Makofske; Joseph Michalewsky; Joseph Triscari; David L. Nelson; Sally Weatherford


Journal of Medicinal Chemistry | 1992

Analogs of CCK incorporating conformationally constrained replacements for Asp32.

Jefferson Wright Tilley; Waleed Danho; Madison; Fry D; Joseph Swistok; Raymond C. Makofske; Joseph Michalewsky; Schwartz A; Sally Weatherford; Joseph Triscari


Archive | 2011

GLUCOSE-DEPENDENT INSULINOTROPIC PEPTIDE ANALOGS

Waleed Danho; George Ehrlich; Wajiha Khan; Joseph Swistok; Jefferson Wright Tilley


Archive | 2006

Peptide mit neuropeptide-2 rezeptor agonist aktivität Peptides neuropeptide-2 receptor agonist activity

Waleed Danho; George Ehrlich; David C. Fry; Wajiha Khan; Joseph Swistok


Archive | 2006

Peptides with agonist activity of neuropeptide-2 receptor (Y2R).

Waleed Danho; George Ehrlich; David C. Fry; Wajiha Khan; Joseph Swistok

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Joseph Swistok

University of Texas Southwestern Medical Center

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