NDLI: MAFA and T3 Drive Maturation of Both Fetal Human Islets and Insulin-Producing Cells Differentiated From hESC.

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MAFA and T3 Drive Maturation of Both Fetal Human Islets and Insulin-Producing Cells Differentiated From hESC.

Content Provider	World Health Organization (WHO)-Global Index Medicus
Author	Aguayo-Mazzucato, Cristina Cahill, Christopher Hollister-Lock, Jennifer Weir, Gordon Sharma, Arun Colton, Clark Bonner-Weir, Susan DiIenno, Amanda
Description	Author Affiliation: Aguayo-Mazzucato C ( Joslin Diabetes Center (C.A.-M., J.H.-L., C.Ca., A.S., G.W., S.B.-W.), Harvard Medical School, Boston, Massachusetts 02215); DiIenno A ( Joslin Diabetes Center (C.A.-M., J.H.-L., C.Ca., A.S., G.W., S.B.-W.), Harvard Medical School, Boston, Massachusetts 02215); Hollister-Lock J ( Joslin Diabetes Center (C.A.-M., J.H.-L., C.Ca., A.S., G.W., S.B.-W.), Harvard Medical School, Boston, Massachusetts 02215); Cahill C ( Joslin Diabetes Center (C.A.-M., J.H.-L., C.Ca., A.S., G.W., S.B.-W.), Harvard Medical School, Boston, Massachusetts 02215); Sharma A ( Joslin Diabetes Center (C.A.-M., J.H.-L., C.Ca., A.S., G.W., S.B.-W.), Harvard Medical School, Boston, Massachusetts 02215); Weir G ( Joslin Diabetes Center (C.A.-M., J.H.-L., C.Ca., A.S., G.W., S.B.-W.), Harvard Medical School, Boston, Massachusetts 02215); Colton C ( Joslin Diabetes Center (C.A.-M., J.H.-L., C.Ca., A.S., G.W., S.B.-W.), Harvard Medical School, Boston, Massachusetts 02215); Bonner-Weir S ( Joslin Diabetes Center (C.A.-M., J.H.-L., C.Ca., A.S., G.W., S.B.-W.), Harvard Medical School, Boston, Massachusetts 02215)
Abstract	CONTEXT: Human embryonic stem cells (hESCs) differentiated toward ß-cells and fetal human pancreatic islet cells resemble each other transcriptionally and are characterized by immaturity with a lack of glucose responsiveness, low levels of insulin content, and impaired proinsulin-to-insulin processing. However, their response to stimuli that promote functionality have not been compared. OBJECTIVE: The objective of the study was to evaluate the effects of our previous strategies for functional maturation developed in rodents in these two human models of ß-cell immaturity and compare their responses. Design, Settings, Participants, and Interventions: In proof-of-principle experiments using either adenoviral-mediated overexpression of V-Maf avian musculoaponeurotic fibrosarcoma oncogene homolog A (MAFA) or the physiologically driven path via thyroid hormone (T3) and human fetal islet-like cluster (ICC) functional maturity was evaluated. Then the effects of T3 were evaluated upon the functional maturation of hESCs differentiated toward ß-cells. MAIN OUTCOME MEASURES: Functional maturation was evaluated by the following parameters: glucose responsiveness, insulin content, expression of the mature ß-cell transcription factor MAFA, and proinsulin-to-insulin processing. RESULTS: ICCs responded positively to MAFA overexpression and T3 treatment as assessed by two different maturation parameters: increased insulin secretion at 16.8 mM glucose and increased proinsulin-to-insulin processing. In hESCs differentiated toward ß-cells, T3 enhanced MAFA expression, increased insulin content (probably mediated by the increased MAFA), and increased insulin secretion at 16.8 mM glucose. CONCLUSION: T3 is a useful in vitro stimulus to promote human ß-cell maturation as shown in both human fetal ICCs and differentiated hESCs. The degree of maturation induced varied in the two models, possibly due to the different developmental status at the beginning of the study.
ISSN	0021972X
e-ISSN	19457197
Journal	The Journal of Clinical Endocrinology & Metabolism
Issue Number	10
Volume Number	100
Language	English
Publisher	Oxford University Press
Publisher Date	2015-10-01
Publisher Place	United States
Access Restriction	Open
Subject Keyword	Cell Differentiation Physiology Embryonic Stem Cells Metabolism Insulin-secreting Cells Islets Of Langerhans Maf Transcription Factors, Large Triiodothyronine Pharmacology Drug Effects Cytology Glucose Insulin Genetics Research Support, N.i.h., Extramural Research Support, Non-u.s. Gov't Discipline Endocrinology Discipline Metabolism
Content Type	Text
Resource Type	Article
Subject	Biochemistry (medical) Endocrinology, Diabetes and Metabolism Clinical Biochemistry Biochemistry Endocrinology

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