کد مقاله کد نشریه سال انتشار مقاله انگلیسی نسخه تمام متن
5534116 1550825 2017 8 صفحه PDF دانلود رایگان
عنوان انگلیسی مقاله ISI
Key amino acid residue in Melanocortin-1 receptor (melanocyte α-MSH receptor) for ligand selectivity
موضوعات مرتبط
علوم زیستی و بیوفناوری بیوشیمی، ژنتیک و زیست شناسی مولکولی بیولوژی سلول
پیش نمایش صفحه اول مقاله
Key amino acid residue in Melanocortin-1 receptor (melanocyte α-MSH receptor) for ligand selectivity
چکیده انگلیسی


- MC1R is a subtype of the melanocortin receptor family and NDP-α-MSH is an agonist at MC1R and MC4R but des-Trp9-NDP-α-MSH loses agonist activity at MC4R.
- TM3 of MCRs is involved in des-Trp9-NDP-α-MSH selectivity.
- Mutation M128 in TM3 of MC1R reduced des-Trp9-NDP-α-MSH agonist activity.

The melanocortin-1 receptor (MC1R) is a subtype of the melanocortin receptor family and NDP-α-MSH is a non-selective agonist for MC1R. The core sequence of NDP-α-MSH, His-Phe-Arg-Trp, is important for ligand binding and biological activities at the melanocortin receptor subtypes (MCRs). A recent study indicates that Trp9 in NDP-α-MSH plays an important role in ligand selectivity. Deletion of Trp9 in NDP-α−MSH (des-Trp9-NDP-α-MSH) resulted in loss of agonist activity at MC4R, although remains agonist activity at MC1R. The molecular basis for this receptor ligand selectivity is unknown. In this study we examined what region of the MC1R is responsible for des-NDP-α-MSH selectivity. Our results indicate that (1) substitution of TM3 of MC4R with the corresponding region of MC1R switches des-Trp9-NDP-α-MSH from no activity to agonist; (2) des-Trp9-NDP-α-MSH exhibits agonistic activity at the L133M mutation of the MC4R; and (3) substitution of non-conserved amino acid residue M128 in TM3 of MC1R significantly reduced des-Trp9-NDP-α-MSH agonist activity. Our results demonstrate that amino acid residue 128 in TM3 of MC1R, or amino acid residue L133 in TM3 of the MC4R, play crucial roles in ligand des-Trp9-NDP-α-MSH selectivity at MC1R or MC4R.

ناشر
Database: Elsevier - ScienceDirect (ساینس دایرکت)
Journal: Molecular and Cellular Endocrinology - Volume 454, 15 October 2017, Pages 69-76
نویسندگان
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