DOES FOLIC ACID SUPPLEMENTATION PREVENT NICOTINE-INDUCED BETA CELL DYSFUNCTION

Nicholson, Catherine J.

Please use this identifier to cite or link to this item: http://hdl.handle.net/11375/12875

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DC Field	Value	Language
dc.contributor.advisor	Holloway, Alison C	en_US
dc.contributor.advisor	Raha, Sandeep	en_US
dc.contributor.advisor	McDonald, Sarah	en_US
dc.contributor.author	Nicholson, Catherine J.	en_US
dc.date.accessioned	2014-06-18T17:01:03Z	-
dc.date.available	2014-06-18T17:01:03Z	-
dc.date.created	2013-03-01	en_US
dc.date.issued	2013-04	en_US
dc.identifier.other	opendissertations/7724	en_US
dc.identifier.other	8786	en_US
dc.identifier.other	3816390	en_US
dc.identifier.uri	http://hdl.handle.net/11375/12875	-
dc.description.abstract	<p>Previous studies suggest that nicotine impairs pancreatic function, which may explain the increased risk of T2DM in smokers. We have previously shown that nicotine exposure results in decreased beta cell function, an effect which appears to be mediated via increased beta cell oxidative stress. The goal of this study is to determine whether folic acid, an antioxidant, can prevent nicotine-induced beta cell dysfunction in the beta cell.</p> <p>INS 1E cells, a rat pancreatic beta cell line, were treated with nicotine or vehicle ± 10µM folic acid for 48 hours. Nicotine treatment decreased both basal and glucose stimulated insulin secretion, but had no effect on insulin content, mitochondrial function or markers of apoptosis. Expression of oxidative stress/damage markers (HSP70 and 4-HNE), antioxidant enzymes (Cu/ZnSOD, MnSOD and CAT), insulin gene transcription factor PDX1 and K<sub>ATP </sub>channel subunit kir<sub>6.2</sub> were determined by western blot analysis. Expression of HSP70, 4-HNE and MnSOD were significantly increased with nicotine treatment (p=0.002, 0.05 and 0.03 respectively). Cu/ZnSOD and CAT expression remained unchanged with nicotine treatment. The addition of folic acid significantly reduced HSP70 expression, 4-HNE expression, CAT expression, but did not alter the expression of MnSOD. There was a significant (p6.2expression (p=0.019) which showed a trend toward reduced expression following treatment with folic acid (p=0.067).</p> <p>Nicotine treatment significantly increases markers of oxidative stress and oxidative damage in pancreatic beta cells; an effect which was reversed by folic acid administration. Nicotine and folic acid treatment increased insulin content, likely mediated through an increase in the insulin gene transcription factor, PDX1. Furthermore, nicotine treatment increased expression of kir<sub>6.2, </sub>suggesting a defect in the insulin secretory mechanism. This effect was reversed with folic acid treatment.Although many studies suggest that Canadians are meeting or exceeding recommended folate levels, this is not true in smokers. Our data suggest that additional folate supplementation in smokers may prevent nicotine-induced damage to the pancreas and thus reduce the risk of type 2 diabetes.</p>	en_US
dc.subject	Diabetes	en_US
dc.subject	Beta cell	en_US
dc.subject	Beta cell dysfunction	en_US
dc.subject	nicotine	en_US
dc.subject	Folic acid	en_US
dc.subject	Chemical and Pharmacologic Phenomena	en_US
dc.subject	Medical Pharmacology	en_US
dc.subject	Medical Physiology	en_US
dc.subject	Chemical and Pharmacologic Phenomena	en_US
dc.title	DOES FOLIC ACID SUPPLEMENTATION PREVENT NICOTINE-INDUCED BETA CELL DYSFUNCTION	en_US
dc.type	thesis	en_US
dc.contributor.department	Medical Sciences (Division of Physiology/Pharmacology)	en_US
dc.description.degree	Master of Science (MSc)	en_US
Appears in Collections:	Open Access Dissertations and Theses

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