Secretion from adipose cells

	Associate Provost for Research Boston University Medical Campus
NIDDK - National Institute of Diabetes & Digestive & Kidney Diseases	Research Resources

Abstract

Grant Number:	5R01DK056736-06
PI Name:	KANDROR, KONSTANTIN V.
PI Email:	kandror@biochem.bumc.bu.edu
PI Title:	ASSOCIATE PROFESSOR
Project Title:	Secretion from adipose cells

Abstract: DESCRIPTION (provided by applicant): As the prevalence of obesity is rapidly growing in this country and throughout the world, understanding the mechanisms of weight control becomes an urgent biomedical problem. The adipose-derived hormone, leptin, plays a central role in regulation of body weight and energy expenditure. Food intake and accumulation of energy stores in adipocytes result in an increase in leptin production thus leading to inhibition of appetite and elevation of energy expenditure. Conversely, when fat stores decline, adipocytes reduce leptin production, and food intake is increased. However, the biochemical connection between nutrient intake/storage in adipocytes and the level of leptin secretion remains largely unknown. In the previous funding period, we found that production of leptin is regulated at the level of translation via the mTOR-mediated pathway as well as at the level of secretion. Since mTOR (mammalian target of rapamycin) represents a nutrient sensor in the cell, the first pathway may provide a long sought after physiological connection between food intake and leptin expression. Thus, our first goal for the next funding period is to determine how to manipulate expression levels of leptin mRNA stored in adipose cells using specific nutrient signals. For that, we propose to explore the mTOR-mediated mechanism of the translational control of leptin mRNA by various nutrients. This will give us the opportunity to maintain high levels of circulating endogenous leptin without increasing fat stores in adipocytes. Our second goal is to understand the molecular mechanisms of secretion from adipose cells. In particular, we will test the hypothesis that newly discovered Golgi-localized, gamma-ear-containing, Arf-binding proteins participate in the formation of secretory vesicles in adipocytes and regulate secretion from these cells. We will also determine whether or not Glut4-vesicles contain novel secreted proteins as their soluble cargo and continue our search for novel proteins secreted from adipocytes.

Thesaurus Terms:
adipocyte, hormone regulation /control mechanism, intracellular transport, leptin, nutrient requirement
ADP ribosylation, Golgi apparatus, glucose transporter, insulin, membrane protein, protein localization, protein structure function, secretory protein, sirolimus, transcription factor, vesicle /vacuole
genetically modified animal, laboratory mouse, laboratory rat, nutrition related tag, tissue /cell culture

Institution: BOSTON UNIVERSITY MEDICAL CAMPUS

715 ALBANY ST, 560

BOSTON, MA 021182394

Fiscal Year: 2006

Department: BIOCHEMISTRY

Project Start: 01-MAR-2000

Project End: 28-FEB-2010

ICD: NATIONAL INSTITUTE OF DIABETES AND DIGESTIVE AND KIDNEY DISEASES

IRG: CADO

Boston, Tue, 23 Jan 2007 18:55:18 EST

Institution:	BOSTON UNIVERSITY MEDICAL CAMPUS
	715 ALBANY ST, 560
	BOSTON, MA 021182394
Fiscal Year:	2006
Department:	BIOCHEMISTRY
Project Start:	01-MAR-2000
Project End:	28-FEB-2010
ICD:	NATIONAL INSTITUTE OF DIABETES AND DIGESTIVE AND KIDNEY DISEASES
IRG:	CADO