| کد مقاله | کد نشریه | سال انتشار | مقاله انگلیسی | نسخه تمام متن |
|---|---|---|---|---|
| 8348123 | 1541713 | 2015 | 17 صفحه PDF | دانلود رایگان |
عنوان انگلیسی مقاله ISI
A structure-function study of PACAP using conformationally restricted analogs: Identification of PAC1 receptor-selective PACAP agonists
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کلمات کلیدی
VIPT47D cells3T3PAC1-RPACAP38Structure–function studyPACAP27GRPPLCPACAPGHRHEC50PBSIC50DTTbovine serum albumin fraction VIBMXFBSDMEM3-isobutyl-1-methylxanthine - 3-ایزوبوتیل-1-متیلکسانتینBSA - BSAcAMP - cAMPinositol phosphate - inositol فسفاتTraumatic brain injury - آسیب تروماتیک مغزDulbecco's minimum essential medium - حداقل کالای ضروری DulbeccoCNS - دستگاه عصبی مرکزیdithiothreitol - دیتیوتریتولfetal bovine serum - سرم جنین گاوmouse embryonic fibroblast cells - سلول های فیبروبلاست جنین موشStroke - سکته مغزیcentral nervous system - سیستم عصبی مرکزیphospholipase C - فسفولیپاز CNeuroprotection - محافظت نورونی یا محافظت از عصبPhosphate-buffered saline - محلول نمک فسفات با خاصیت بافریhalf-maximal inhibitory concentration - نیمه حداکثر غلظت مهاریgrowth hormone-releasing hormone - هورمون آزاد کننده هورمون رشدpituitary adenylate cyclase-activating polypeptide - پلیپپتید فعال آدنیلات سیکلاس هیپوفیزgastrin-releasing peptide - پپتید آزاد کننده گاسترینvasoactive intestinal peptide - پپتید روده روده ای
موضوعات مرتبط
علوم زیستی و بیوفناوری
بیوشیمی، ژنتیک و زیست شناسی مولکولی
زیست شیمی
پیش نمایش صفحه اول مقاله
چکیده انگلیسی
Pituitary adenylate cyclase-activating polypeptide (PACAP) has widespread physiological/pathophysiological actions and there is increased interest for its use therapeutically, especially in the CNS (neuroprotection). Unfortunately, no selective PACAP-analogs exist for PACAP-preferring PAC1-receptors, primarily because of its high sequence identity to VIP and particularly, because of the inability of structure-function studies to separate the pharmacophore of PAC1-R from VPAC1-R, which has high affinity for PACAP and VIP. The present study attempted to develop PAC1-R-selective agonists primarily by making conformationally restricted PACAP-analogs in positions important for receptor-selectivity/affinity. Forty-six PACAP-related-analogs were synthesized with substitutions in positions 1-4, 14-17, 20-22, 28, 34, 38 and receptor-selectivity determined in PAC1-R,VPAC1-R,VPAC2-R-transfected or native cells from binding or cAMP-generation experiments. Fifteen PACAP-analogs had 6-78-fold higher affinities for PAC1-R than VPAC1-R and 13 were agonists. Although binding-affinities correlated significantly with agonist potency, the degree of receptor-spareness varied markedly for the different PACAP-analogs, resulting in selective potencies for activating the PAC1 receptor over the VPAC1 receptor from 0- to 103-fold. In addition, a number of PACAP-analogs were identified that had high selectivity for PAC1-R over VPAC2-R as well as PACAP-analogs that could prove more useful therapeutically because of substitutions known to extend their half-lives (substitutions at potential sites of proteolysis and attachment of long-chain fatty acids). This study provides for the first time a separation of the pharmacophores for PAC1-R and VPAC1-R, resulting in PACAP-related analogs that are PAC1-R-preferring. Some of these analogs, or their modifications, could prove useful as therapeutic agents for various diseases.
ناشر
Database: Elsevier - ScienceDirect (ساینس دایرکت)
Journal: Peptides - Volume 66, April 2015, Pages 26-42
Journal: Peptides - Volume 66, April 2015, Pages 26-42
نویسندگان
Irene Ramos-Álvarez, Samuel A. Mantey, Taichi Nakamura, Bernardo Nuche-Berenguer, Paola Moreno, Terry W. Moody, Jerome L. Maderdrut, David H. Coy, Robert T. Jensen,