Insulin receptor isoforms: an integrated view focused on gestational diabetes mellitus
Author
dc.contributor.author
Westermeier, Francisco
Author
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Sáez, T.
Author
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Arroyo, P.
Author
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Toledo, F.
Author
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Gutiérrez, J.
Author
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Sanhueza, C.
Author
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Pardo, F.
Author
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Leiva, A.
Author
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Sobrevia, L.
Admission date
dc.date.accessioned
2016-10-18T20:38:49Z
Available date
dc.date.available
2016-10-18T20:38:49Z
Publication date
dc.date.issued
2016
Cita de ítem
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Diabetes Metab Res Rev 2016; 32: 350–365.
es_ES
Identifier
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10.1002/dmrr.2729
Identifier
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https://repositorio.uchile.cl/handle/2250/140870
Abstract
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The human insulin receptor (IR) exists in two isoforms that differ by the absence (IR-A) or the presence (IR-B) of a 12-amino acid segment encoded by exon 11. Both isoforms are functionally distinct regarding their binding affinities and intracellular signalling. However, the underlying mechanisms related to their cellular functions in several tissues are only partially understood. In this review, we summarize the current knowledge in this field regarding the alternative splicing of IR isoform, tissue-specific distribution and signalling both in physiology and disease, with an emphasis on the human placenta in gestational diabetes mellitus (GDM). Furthermore, we discuss the clinical relevance of IR isoforms highlighted by findings that show altered insulin signalling due to differential IR-A and IR-B expression in human placental endothelium in GDM pregnancies. Future research and clinical studies focused on the role of IR isoform signalling might provide novel therapeutic targets for treating GDM to improve the adverse maternal and neonatal outcomes.
es_ES
Patrocinador
dc.description.sponsorship
Fondo Nacional de Desarrollo Cientifico y Tecnologico (FONDECYT), Chile
1150377
1150344
3140532
3130583
3140516
Comision Nacional de Investigacion Cientifica y Tecnologica (CONICYT)-PhD (Chile) fellowship