Co-chaired by Jürgen
Wess, NIDDK and Derek LeRoith, NIDDK
Conference Room E1/E2, Natcher Conference
Center
The growing epidemic of obesity-associated
type 2 diabetes represents one of the major threats to
human health in the 21st century. To gain insight into
the pathophysiology of type 2 diabetes and to develop
new treatment protocols, it is essential to characterize
the molecular components and signaling networks critical
for beta-cell function and glucose and energy homeostasis.
During the past few years, NIH researchers have used
gene targeting and transgenic techniques to develop novel
mouse models to study the molecular basis of type 2 diabetes
and glucose and energy homeostasis. Phenotypical analysis
of these mutant animals has led to a wealth of novel
findings, including the identification of receptors,
G proteins, and other signaling molecules that play key
roles in these processes. Given the preeminent importance
of this topic, this mini-symposium
should be timely and of great interest for a wide audience.
Program:
A Mouse Model of Type 2 Diabetes: Pathophysiology and
Therapeutic Implications
Derek LeRoith, NIDDK
Role of M3 Muscarinic Acetylcholine Receptors in the
Regulation of Body Weight, Beta-cell Function, and Glucose
Homeostasis
Jürgen Wess, NIDDK
Role of the Gnas Locus in the Regulation of Energy and
Glucose Metabolism
Lee S. Weinstein, NIDDK
Cytokine-mediated Stat5 Signaling Is Required for Insulin
Secretion and Glucose Homeostasis
Lothar Hennighausen,
NIDDK
Role of Cyclic Nucleotide Phosphodiesterase 3B (PDE3B)
in Regulation of Energy Homeostasis
Vincent C. Manganiello,
NHLBI
The Hexosamine Signaling Pathway and Diabetes Mellitus
John
A. Hanover, NIDDK
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