A Novel Peptide COX 52-69  Inhibits High Glucose-induced Insulin Secretion by Modulating BK Channel Activity

Qian Lin; Jingtao Liu; Hengling Chen; Wenwu Hu; Weiqiong Lei; Meijie Wang; Xianguang Lin; Yongning Zhang; Huiting Ai; Su Chen; Chenhong Li

doi:10.2174/0113892037249620231010063637

A Novel Peptide COX_52-69 Inhibits High Glucose-induced Insulin Secretion by Modulating BK Channel Activity

Авторлар: Lin Q.¹, Liu J.¹, Chen H.², Hu W.³, Lei W.¹, Wang M.⁴, Lin X.¹, Zhang Y.², Ai H.², Chen S.¹, Li C.²
Мекемелер:
1. Laboratory of Membrane Ion Channels and Medicine, Key Laboratory of Cognitive Science of State Ethnic Affairs Commission, Hubei Key Laboratory of Medical Information Analysis and Tumor Diagnosis and Treatment, College of Biomedical Engineering, South-Central Minzu University
2. Laboratory of Membrane Ion Channels and Medicine, Key Laboratory of Cognitive Science of State Ethnic Affairs Commission, Hubei Key Laboratory of Medical Information Analysis and Tumor Diagnosis and Treatment, College of Biomedical Engineering,, South-Central Minzu University
3. Laboratory of Membrane Ion Channels and Medicine, Key Laboratory of Cognitive Science of State Ethnic Affairs Commission, Hubei Key Laboratory of Medical Information Analysis and Tumor Diagnosis and Treatment, College of Biomedical Engineering, South-Central Minzu University,
4. Laboratory of Membrane Ion Channels and Medicine, Key Laboratory of Cognitive Science of State Ethnic Affairs Commission, Hubei Key Laboratory of Medical Information Analysis and Tumor Diagnosis and Treatment, College of Biomedical Engineering,, South-Central Minzu University,
Шығарылым: Том 25, № 5 (2024)
Беттер: 419-426
Бөлім: Life Sciences
URL: https://rjpbr.com/1389-2037/article/view/645634
DOI: https://doi.org/10.2174/0113892037249620231010063637
ID: 645634

Дәйексөз келтіру

Толық мәтін

Аннотация
Авторлар туралы
Әдебиет тізімі
Қосымша файлдар
Статистика

Аннотация

Background:Excessive insulin is the leading cause of metabolic syndromes besides hyperinsulinemia. Insulin-lowering therapeutic peptides have been poorly studied and warrant urgent attention.

Objective:The main purpose of this study, was to introduce a novel peptide COX52-69 that was initially isolated from the porcine small intestine and possessed the ability to inhibit insulin secretion under high-glucose conditions by modulating large conductance Ca2+-activated K+ channels (BK channels) activity.

Methods and Results:Enzyme-linked immunosorbent assay results indicate that COX52-69 supressed insulin release induced by high glucose levels in pancreatic islets and animal models. Furthermore, electrophysiological data demonstrated that COX52-69 can increase BK channel currents and hyperpolarize cell membranes. Thus, cell excitability decreased, corresponding to a reduction in insulin secretion.

Conclusion:Our study provides a novel approach to modulate high glucose-stimulated insulin secretion in patients with hyperinsulinemia.

Негізгі сөздер

COX&, lt, sub&, gt, 52-69<, /sub&, gt, Insulin secretion, BK channel, pancreatic islets, hyperpolarize cell membranes, hyperinsulinemia.

Авторлар туралы

Qian Lin

Laboratory of Membrane Ion Channels and Medicine, Key Laboratory of Cognitive Science of State Ethnic Affairs Commission, Hubei Key Laboratory of Medical Information Analysis and Tumor Diagnosis and Treatment, College of Biomedical Engineering, South-Central Minzu University

Email: info@benthamscience.net

Әдебиет тізімі

Moreau, F.; Kirk, N.S.; Zhang, F.; Gelfanov, V.; List, E.O.; Chrudinová, M.; Venugopal, H.; Lawrence, M.C.; Jimenez, V.; Bosch, F.; Kopchick, J.J.; DiMarchi, R.D.; Altindis, E.; Kahn, C.R. Interaction of a viral insulin-like peptide with the IGF-1 receptor produces a natural antagonist. Nat. Commun., 2022, 13(1), 6700. doi: 10.1038/s41467-022-34391-6 PMID: 36335114
Templeman, N.M.; Skovsø, S.; Page, M.M.; Lim, G.E.; Johnson, J.D. A causal role for hyperinsulinemia in obesity. J. Endocrinol., 2017, 232(3), R173-R183. doi: 10.1530/JOE-16-0449 PMID: 28052999
Elena, M.; Chu, A. Pediatr. Ann., 2017, 46(11), e409. PMID: 29131920
(a) Dongerkery, S.P.; Schroeder, P.R.; Shomali, M.E. Insulin and its cardiovascular effects: What is the current evidence? Curr. Diab. Rep., 2017, 17(12), 120. doi: 10.1007/s11892-017-0955-3 PMID: 29058131; (b) Poirier, P.; Giles, T.D.; Bray, G.A.; Hong, Y.; Stern, J.S.; Pi-Sunyer, F.X.; Eckel, R.H. Obesity and cardiovascular disease: Pathophysiology, evaluation, and effect of weight loss. Circulation, 2006, 113(6), 898-918. doi: 10.1161/CIRCULATIONAHA.106.171016 PMID: 16380542; (c) Hamano, K.; Akita, K.; Takeuchi, Y.; Suwa, T.; Takeda, J.; Dodo, S. Glucose-responsive Insulinoma with Insulin Hypersecretion Suppressed by Metformin. Intern. Med., 2019, 58(24), 3563-3568. doi: 10.2169/internalmedicine.3318-19 PMID: 31462593
Perry, R.J.; Shulman, G.I. Mechanistic links between obesity, insulin, and cancer. Trends Cancer, 2020, 6(2), 75-78. doi: 10.1016/j.trecan.2019.12.003 PMID: 32061306
Hopkins, B.D.; Goncalves, M.D.; Cantley, L.C. InsulinPI3K signalling: An evolutionarily insulated metabolic driver of cancer. Nat. Rev. Endocrinol., 2020, 16(5), 276-283. doi: 10.1038/s41574-020-0329-9 PMID: 32127696
(a) Dahiya, R.; Dahiya, S.; Kumar, P.; Kumar, R.V.; Dahiya, S.; Kumar, S.; Saharan, R.; Basu, P.; Mitra, A.; Sharma, A.; Kashaw, S.K.; Patel, J.K. Structural and biological aspects of natural bridged macrobicyclic peptides from marine resources. Arch. Pharm. (Weinheim), 2021, 354(8), 2100034. doi: 10.1002/ardp.202100034 PMID: 33913195; (b) Dahiya, R.; Dahiya, S.; Fuloria, N.K.; Mourya, R.; Dahiya, S.; Fuloria, S.; Kumar, S.; Shrivastava, J.; Saharan, R.; Chennupati, S.V.; Patel, J.K. Natural Bridged Bicyclic Peptide Macrobiomolecules from Celosia argentea and Amanita phalloides. Mini Rev. Med. Chem., 2022, 22(13), 1772-1788. doi: 10.2174/1389557522666220113122117 PMID: 35049431; (c) Muttenthaler, M.; King, G.F.; Adams, D.J.; Alewood, P.F. Trends in peptide drug discovery. Nat. Rev. Drug Discov., 2021, 20(4), 309-325. doi: 10.1038/s41573-020-00135-8 PMID: 33536635
(a) Hansen, P.R.; Oddo, A. Fmoc Solid-Phase Peptide Synthesis. Methods Mol. Biol., 2015, 1348, 33-50. doi: 10.1007/978-1-4939-2999-3_5 PMID: 26424261; (b) Chan, W. C.; White, P. D. Fmoc Solid-Phase Peptide Synthesis: A Practical Approach., 2000.
Chen, Z.; Agerberth, B.; Gell, K.; Andersson, M.; Mutt, V.; Ostenson, C.G.; Efendić, S.; Barros-Söderling, J.; Persson, B.; Jörnvall, H. Isolation and characterization of porcine diazepam-binding inhibitor, a polypeptide not only of cerebral occurrence but also common in intestinal tissues and with effects on regulation of insulin release. Eur. J. Biochem., 1988, 174(2), 239-244. doi: 10.1111/j.1432-1033.1988.tb14088.x PMID: 3289918
(a) Xie, L.; Lu, J.; Östenson, C.G.; Xu, T.; Chen, Z.W. GIP139, a novel insulinotropic peptide form and aspects on its mechanism of action. Regul. Pept., 2004, 121(1-3), 107-112. doi: 10.1016/j.regpep.2004.04.013 PMID: 15256280; (b) Wang, J.; Zeng, Y.; Yan, D.; Lu, J.; Chen, Z.; Li, C. Purification and characterization of novel truncated fragments of bioactive proteins from porcine intestine with effects on insulin secretion. Sci. Res. Essays, 2012, 7(34), 3026-3031. doi: 10.5897/SRE12.033
(a) Bachem, M.G.; Schneider, E.; Groß, H.; Weidenbach, H.; Schmid, R.M.; Menke, A.; Siech, M.; Beger, H.; Grünert, A.; Adler, G. Identification, culture, and characterization of pancreatic stellate cells in rats and humans. Gastroenterology, 1998, 115(2), 421-432. doi: 10.1016/S0016-5085(98)70209-4 PMID: 9679048; (b) Velasco, M.; Larqué, C.; Díaz-García, C.M.; Sanchez-Soto, C.; Hiriart, M. Rat pancreatic beta-cell culture. Methods Mol. Biol., 2018, 1727, 261-273. doi: 10.1007/978-1-4939-7571-6_20 PMID: 29222788
(a) Leung, Y.M.; Ahmed, I.; Sheu, L.; Tsushima, R.G.; Diamant, N.E.; Hara, M.; Gaisano, H.Y. Electrophysiological characterization of pancreatic islet cells in the mouse insulin promoter-green fluorescent protein mouse. Endocrinology, 2005, 146(11), 4766-4775. doi: 10.1210/en.2005-0803 PMID: 16109783; (b) Houamed, K.M.; Sweet, I.R.; Satin, L.S. BK channels mediate a novel ionic mechanism that regulates glucose-dependent electrical activity and insulin secretion in mouse pancreatic β-cells. J. Physiol., 2010, 588(18), 3511-3523. doi: 10.1113/jphysiol.2009.184341 PMID: 20643769
Visa, M.; Alcarraz-Vizán, G.; Montane, J.; Cadavez, L.; Castaño, C.; Villanueva-Peñacarrillo, M.L.; Servitja, J.M.; Novials, A. Islet amyloid polypeptide exerts a novel autocrine action in β-cell signaling and proliferation. FASEB J., 2015, 29(7), 2970-2979. doi: 10.1096/fj.15-270553 PMID: 25808537
(a) Drews, G.; Krippeit-Drews, P.; Düfer, M. Electrophysiology of islet cells. Adv. Exp. Med. Biol., 2010, 654, 115-163. doi: 10.1007/978-90-481-3271-3_7 PMID: 20217497; (b) Göpel, S.O.; Kanno, T.; Barg, S.; Weng, X.G.; Gromada, J.; Rorsman, P. Regulation of glucagon release in mouse α-cells by K ATP channels and inactivation of TTX-sensitive Na + channels. J. Physiol., 2000, 528(3), 509-520. doi: 10.1111/j.1469-7793.2000.00509.x PMID: 11060128; (c) Remedi, M.S.; Rocheleau, J.V.; Tong, A.; Patton, B.L.; McDaniel, M.L.; Piston, D.W.; Koster, J.C.; Nichols, C.G. Hyperinsulinism in mice with heterozygous loss of KATP channels. Diabetologia, 2006, 49(10), 2368-2378. doi: 10.1007/s00125-006-0367-4 PMID: 16924481
(a) Nakashima, K.; Kanda, Y.; Hirokawa, Y.; Kawasaki, F.; Matsuki, M.; Kaku, K. MIN6 is not a pure beta cell line but a mixed cell line with other pancreatic endocrine hormones. Endocr. J., 2009, 56(1), 45-53. doi: 10.1507/endocrj.K08E-172 PMID: 18845907; (b) Yamato, E.; Tashiro, F.; Miyazaki, J. Microarray analysis of novel candidate genes responsible for glucose-stimulated insulin secretion in mouse pancreatic β-cell line MIN6. PLoS One, 2013, 8(4), e61211. doi: 10.1371/journal.pone.0061211 PMID: 23560115
(a) Latorre, R.; Castillo, K.; Carrasquel-Ursulaez, W.; Sepulveda, R.V.; Gonzalez-Nilo, F.; Gonzalez, C.; Alvarez, O. Molecular determinants of BK channel functional diversity and functioning. Physiol. Rev., 2017, 97(1), 39-87. doi: 10.1152/physrev.00001.2016 PMID: 27807200; (b) Shangjian, L.; Zhengrong, D.; Liqiang, W.; Lei, L.; Wenting, A.; Xiling, S.; Xinyi, C. Reduction of large-conductance Ca2+-activated K+ channel with compensatory increase of nitric oxide in insulin resistant rats. Diabetes Metab. Res. Rev., 2011, 27(5), 461-469. doi: 10.1002/dmrr.1196 PMID: 21425425; (c) Neves, C.; Milton, G.; Cesaretti, M.; Kohlmann, N.; Agostinho, T.; Zanella, M.T.; Ribeiro, A.B.; Osvaldo, K. Am. J. Hypertens., (S1), A218-A218.; (d) Chamberlain, L.H.; Shipston, M.J.; Gould, G.W. Regulatory effects of protein S-acylation on insulin secretion and insulin action. Open Biol., 2021, 11(3), 210017. doi: 10.1098/rsob.210017 PMID: 33784857
(a) DeCensi, A.; Puntoni, M.; Goodwin, P.; Cazzaniga, M.; Gennari, A.; Bonanni, B.; Gandini, S. Metformin and cancer risk in diabetic patients: A systematic review and meta-analysis. Cancer Prev. Res. (Phila.), 2010, 3(11), 1451-1461. doi: 10.1158/1940-6207.CAPR-10-0157 PMID: 20947488; (b) Dev, R.; Bruera, E.; Dalal, S. Insulin resistance and body composition in cancer patients. Ann. Oncol., 2018, 29, ii18-ii26. doi: 10.1093/annonc/mdx815
Kim, H.J.; Lee, S.; Chun, K.H.; Jeon, J.Y.; Han, S.J.; Kim, D.J.; Kim, Y.S.; Woo, J-T.; Nam, M-S.; Baik, S.H. Medicine (Baltimore), 2018, 97(8)

Қосымша файлдар

Әрекет

1. JATS XML

Жүктеу

Пайдаланушының аты
Құпиясөз
Мені есте сақтау

Құпия сөзді ұмыттыңыз ба?	Тіркеу

Пайдаланушының аты
Құпиясөз
Мені есте сақтау

Құпия сөзді ұмыттыңыз ба?	Тіркеу