Chronic exposure to GLP-1R agonists promotes homologous GLP-1 receptor desensitization in vitro but does not attenuate GLP-1R-dependent glucose homeostasis in vivo
Glucagon-like peptide-1 (GLP-1) stimulates glucose-dependent insulin secretion and inhibits food intake, gastric emptying, and glucagon secretion, actions that promote reduction of fasting and postprandial glycemia in subjects with type 2 diabetes. The rapid degradation of native GLP-1 has engendere...
Saved in:
| Published in | Diabetes (New York, N.Y.) Vol. 53; no. 12; p. S205 |
|---|---|
| Main Authors | , , |
| Format | Journal Article |
| Language | English |
| Published |
American Diabetes Association
01.12.2004
|
| Subjects | |
| Online Access | Get full text |
| ISSN | 0012-1797 |
Cover
| Abstract | Glucagon-like peptide-1 (GLP-1) stimulates glucose-dependent insulin secretion and inhibits food intake, gastric emptying, and glucagon secretion, actions that promote reduction of fasting and postprandial glycemia in subjects with type 2 diabetes. The rapid degradation of native GLP-1 has engendered interest in more stable longer-acting GLP-1 receptor agonists such as exendin-4 (Ex-4); however, the potential consequences of sustained GLP-1 receptor activation leading to receptor desensitization has not been extensively studied. We have now examined a range of GLP-1 receptor-dependent responses following treatment with Ex-4 using INS-1 cells in vitro and both wild-type control and MT-Ex-4 transgenic mice in vivo. Although both GLP-1 and Ex-4 acutely desensitized GLP-1 receptor-dependent cAMP accumulation in INS-1 cells, Ex-4 produced more sustained receptor desensitization, relative to GLP-1, in both acute (5-120 min) and chronic (24-72 h) experiments. PMA (4-phorbol 12-myristate 13-acetate) but not glucagon, glucose-dependent insulinotropic polypeptide (GIP), or epinephrine produced heterologous desensitization in vitro. MT-Ex-4 transgenic mice exhibited a reduced glycemic response to oral but not intraperitoneal glucose challenge following acute Ex-4 administration. In contrast, no differences in glycemic excursion or plasma insulin were observed after I week of twice-daily Ex-4 administration to wild-type versus MT-Ex-4 mice. Similarly, the levels of insulin, pdx-1, and GLP-1 receptor mRNA transcripts were comparable in wild-type and MT-Ex-4 transgenic mice after 1 week of Ex-4 administration. However, repeated Ex-4 administration significantly reduced food intake in MT-Ex-4 but not in wild-type mice. These findings illustrate that although Ex-4 is more potent than native GLP-1 in producing GLP-1 receptor desensitization in vitro, chronic exposure to Ex-4 in normal or transgenic mice is not associated with significant downregulation of GLP-1 receptor-dependent responses coupled to glucose homeostasis in vivo. |
|---|---|
| AbstractList | Glucagon-like peptide-1 (GLP-1) stimulates glucose-dependent insulin secretion and inhibits food intake, gastric emptying, and glucagon secretion, actions that promote reduction of fasting and postprandial glycemia in subjects with type 2 diabetes. The rapid degradation of native GLP-1 has engendered interest in more stable longer-acting GLP-1 receptor agonists such as exendin-4 (Ex-4); however, the potential consequences of sustained GLP-1 receptor activation leading to receptor desensitization has not been extensively studied. We have now examined a range of GLP-1 receptor-dependent responses following treatment with Ex-4 using INS-1 cells in vitro and both wild-type control and MT-Ex-4 transgenic mice in vivo. Although both GLP-1 and Ex-4 acutely desensitized GLP-1 receptor-dependent cAMP accumulation in INS-1 cells, Ex-4 produced more sustained receptor desensitization, relative to GLP-1, in both acute (5-120 min) and chronic (24-72 h) experiments. PMA (4-phorbol 12-myristate 13-acetate) but not glucagon, glucose-dependent insulinotropic polypeptide (GIP), or epinephrine produced heterologous desensitization in vitro. MT-Ex-4 transgenic mice exhibited a reduced glycemic response to oral but not intraperitoneal glucose challenge following acute Ex-4 administration. In contrast, no differences in glycemic excursion or plasma insulin were observed after I week of twice-daily Ex-4 administration to wild-type versus MT-Ex-4 mice. Similarly, the levels of insulin, pdx-1, and GLP-1 receptor mRNA transcripts were comparable in wild-type and MT-Ex-4 transgenic mice after 1 week of Ex-4 administration. However, repeated Ex-4 administration significantly reduced food intake in MT-Ex-4 but not in wild-type mice. These findings illustrate that although Ex-4 is more potent than native GLP-1 in producing GLP-1 receptor desensitization in vitro, chronic exposure to Ex-4 in normal or transgenic mice is not associated with significant downregulation of GLP-1 receptor-dependent responses coupled to glucose homeostasis in vivo. |
| Audience | Professional |
| Author | Kim, Jung-Guk Baggio, Laurie L Drucker, Daniel J |
| Author_xml | – sequence: 1 fullname: Baggio, Laurie L – sequence: 2 fullname: Kim, Jung-Guk – sequence: 3 fullname: Drucker, Daniel J |
| BookMark | eNp9kMFKAzEQhvdQwVZ9h4AnDytJuia7x1K0CoWK6Lmk2dk1ss2UnVkRX8cXNdIeFIrMYWDm-_9_mEk2ihhhlI2lVDpXtrKn2YToTUppUo2zr_lrjzF4AR87pKEHwSgWy8dcPQnXpg0xiV2PW2Qg8Zp6hy0OtGdEDx52jL2ogSBS4PDpOGAUIYr3wD2KzcCixqSNyMIxQxwcwyEir2EHsYbIou0GjwQ_EYDEjgLtTd7xPDtpXEdwcehn2cvd7fP8Pl-uFg_z2TJvlbU6L5VrisK6yhpz47TX3iuQpfK-KYvpjS21NVrKTVFNpSqNr2pjzUZOnZWgN8pPz7LLvW_rOliH2CD3zm8D-fVMaaN0URmdqPwI1UKE3nXp2U1I4z_89RE-VQ3b4I8Krv4IEsPwwa0biNblYvnfMQfWY9dBC-v0nvnqN_8NqqWk1Q |
| ClassificationCodes | 8000212 541714 8733 541715 8731 |
| ContentType | Journal Article |
| Copyright | COPYRIGHT 2004 American Diabetes Association |
| Copyright_xml | – notice: COPYRIGHT 2004 American Diabetes Association |
| DBID | 8GL |
| DatabaseName | Gale In Context: High School |
| DatabaseTitleList | |
| DeliveryMethod | fulltext_linktorsrc |
| Discipline | Medicine |
| ExternalDocumentID | A126124962 |
| GeographicLocations | United States |
| GeographicLocations_xml | – name: United States |
| GroupedDBID | --- .55 .GJ .XZ 08P 0R~ 18M 29F 2WC 354 4.4 53G 5GY 5RE 5RS 5VS 6PF 7RV 7X7 88E 88I 8AF 8AO 8C1 8F7 8FE 8FH 8FI 8FJ 8G5 8GL 8R4 8R5 AAFWJ AAKAS AAQQT AAWTL AAYEP AAYJJ AAYOK ABOCM ABUWG ACGFO ACGOD ACPRK ADBBV ADZCM AEGXH AENEX AERZD AFFNX AFKRA AHMBA AIAGR AIZAD ALIPV ALMA_UNASSIGNED_HOLDINGS AZQEC BAWUL BBNVY BCR BCU BEC BENPR BES BHPHI BKEYQ BKNYI BLC BPHCQ BTFSW BVXVI C1A CCPQU CS3 DIK DU5 DWQXO E3Z EBS EDB EJD EMOBN EX3 F5P FRP FYUFA GICCO GNUQQ GUQSH GX1 H13 HCIFZ HMCUK HZ~ IAG IAO IEA IHR INH INR IOF IPO ITC J5H K-O K2M K9- KQ8 L7B LK8 M0R M1P M2O M2P M2Q M5~ M7P N4W NAPCQ O9- OB3 OHH OK1 OVD P2P PCD PEA PHGZM PHGZT PMFND PQQKQ PROAC PSQYO Q2X RHI RPM S0X SJFOW SJN SV3 TDI TEORI TR2 UKHRP VVN W8F WH7 WOQ WOW X7M YFH YHG YOC ZGI ZXP ZY1 ~KM |
| ID | FETCH-LOGICAL-g1772-81af447a97665a2c2cc1e081ccf843578276200b4930186c9d676b03a70e2b1c3 |
| ISSN | 0012-1797 |
| IngestDate | Tue Jun 17 22:09:06 EDT 2025 Fri Jun 13 00:08:51 EDT 2025 Tue Jun 10 21:08:45 EDT 2025 Fri Jun 27 05:37:25 EDT 2025 Tue Jun 10 20:00:53 EDT 2025 |
| IsPeerReviewed | true |
| IsScholarly | true |
| Issue | 12 |
| Language | English |
| LinkModel | OpenURL |
| MergedId | FETCHMERGED-LOGICAL-g1772-81af447a97665a2c2cc1e081ccf843578276200b4930186c9d676b03a70e2b1c3 |
| PageCount | 10 |
| ParticipantIDs | gale_infotracmisc_A126124962 gale_infotracgeneralonefile_A126124962 gale_infotracacademiconefile_A126124962 gale_incontextgauss_8GL_A126124962 gale_incontextcollege_GICCO_A126124962 |
| PublicationCentury | 2000 |
| PublicationDate | 20041201 |
| PublicationDateYYYYMMDD | 2004-12-01 |
| PublicationDate_xml | – month: 12 year: 2004 text: 20041201 day: 01 |
| PublicationDecade | 2000 |
| PublicationTitle | Diabetes (New York, N.Y.) |
| PublicationTitleAlternate | Diabetes |
| PublicationYear | 2004 |
| Publisher | American Diabetes Association |
| Publisher_xml | – name: American Diabetes Association |
| SSID | ssj0006060 |
| Score | 1.7557387 |
| Snippet | Glucagon-like peptide-1 (GLP-1) stimulates glucose-dependent insulin secretion and inhibits food intake, gastric emptying, and glucagon secretion, actions that... |
| SourceID | gale |
| SourceType | Aggregation Database |
| StartPage | S205 |
| SubjectTerms | Care and treatment Diabetes Diabetes mellitus Diabetes research Glucagon |
| Title | Chronic exposure to GLP-1R agonists promotes homologous GLP-1 receptor desensitization in vitro but does not attenuate GLP-1R-dependent glucose homeostasis in vivo |
| Volume | 53 |
| hasFullText | 1 |
| inHoldings | 1 |
| isFullTextHit | |
| isPrint | |
| link | http://utb.summon.serialssolutions.com/2.0.0/link/0/eLvHCXMwnV1Lb9QwELaWIiEuiKcoFGQhVA6RUR7O69gXW1VtqUor9bayHSfsJUa7yR74O_xRZtZONhv1ULhkV9mJHWW-nRlPZj4T8lnzIhSRCpnwdcp4ICTLIpEypWAtUchQRyXmIS8uk9NbfnYX300mw6qltpFf1e97-0r-R6twDvSKXbL_oNl-UDgB30G_cAQNw_FBOnbMtkjTbzDTh4Hk9PyKBdeeqAxy4i6xAAu0oZfeT_gEQ4clr2sZD2yd_gVLbq_ADiSs3bItmZgCWc2bhfFk23iFgWtrg12PEF63EJq6KVi3fy6yiti6d5hCGwg3keRkPcjKDIPf40Ged7wD0CAjcSiqam66pu259vr8tNv6-QwMFJu2fY_R8aIvDrEd8-5dV5fM4OPCkO4tVX9DY5A6Mw6XgSVJh2bccg53cA0HRvlH6Mcbd9cXIR4ESJ_Gc_Tgj6IAjOTjw5PLq-vekcPaznYwudmc1x7EHzfPyTO3cKAHFgUvyETXL8mTC1ca8Yr8cWCgHRhoY6jVFO3AQDsw0A0YrAztwEBHYKDzmq7BQAEMFMFAAQy0BwMdg4E6MNABGOwgK_Oa3H47uTk6ZW4HDlYFsOxiWSBKzlMBMWsSi1CFSgUagkilyowjT1IIvtT3Jc_BT2SJyoskTaQPf3ZfhzJQ0RuyU5tavyU0jhMdxGUqgzKHITlYhNzXOk4L6QtdyF2yjw93hpwkNRY9KZs4m8H9HH2fbZS1Sz5tC1aiXS5n2fR8S-iLEypNsxBKuGYTuBfkO9uS3N-SrCzb-32Ce1uCYIbV4Od3Dx3nPXm6Qf4e2WkWrf4AgW0jPzoA_gWX0K5K |
| linkProvider | ProQuest |
| openUrl | ctx_ver=Z39.88-2004&ctx_enc=info%3Aofi%2Fenc%3AUTF-8&rfr_id=info%3Asid%2Fsummon.serialssolutions.com&rft_val_fmt=info%3Aofi%2Ffmt%3Akev%3Amtx%3Ajournal&rft.genre=article&rft.atitle=Chronic+exposure+to+GLP-1R+agonists+promotes+homologous+GLP-1+receptor+desensitization+in+vitro+but+does+not+attenuate+GLP-1R-dependent+glucose+homeostasis+in+vivo&rft.jtitle=Diabetes+%28New+York%2C+N.Y.%29&rft.au=Baggio%2C+Laurie+L&rft.au=Kim%2C+Jung-Guk&rft.au=Drucker%2C+Daniel+J&rft.date=2004-12-01&rft.pub=American+Diabetes+Association&rft.issn=0012-1797&rft.volume=53&rft.issue=12&rft.spage=S205&rft.externalDocID=A126124962 |
| thumbnail_l | http://covers-cdn.summon.serialssolutions.com/index.aspx?isbn=/lc.gif&issn=0012-1797&client=summon |
| thumbnail_m | http://covers-cdn.summon.serialssolutions.com/index.aspx?isbn=/mc.gif&issn=0012-1797&client=summon |
| thumbnail_s | http://covers-cdn.summon.serialssolutions.com/index.aspx?isbn=/sc.gif&issn=0012-1797&client=summon |