Christian Vaisse, MD, PhD

Professor

Diabetes Center

[email protected]

415-514-0530

Linking Cell Signaling and Membrane Traffic

The overall goal of this laboratory is to identify genetic defects implicated in the onset and progression of multi-factorial metabolic diseases such as obesity and diabetes. Our strategy combines human genetic approaches with molecular biology and animal studies.

We are currently concentrating our research on the molecular mechanisms implicated in the hypothalamic effects of the adipocyte secreted, weight regulating hormone, leptin. After describing the first leptin receptor mutation in severely obese humans, we recently found that genetic alterations in the Melanocortin 4 receptor (MC4R), a mediator of the hypothalamic effects of leptin, are responsible for a more common form of human obesity. Using large scale automated screening procedures we now further investigate the frequency of mutations in the MC4R gene in large cohorts of obese patients.

In parallel we also search for obesity causing mutations in additional candidate genes downstream the leptin pathway. Finally, both through in vitro and in vivo studies we are aiming to understand how these mutations cause obesity and what the implications are for the treatment of this condition.

Publications:

Author Correction: Genomic and epigenomic mapping of leptin-responsive neuronal populations involved in body weight regulation.

Postnatal Dynamic Ciliary ARL13B and ADCY3 Localization in the Mouse Brain.

Identification of AgRP cells in the murine hindbrain that drive feeding.

Ciliary ARL13B prevents obesity in mice.

1522-P: Identification of AgRP Cells in the Murine Hindbrain That Drive Feeding.

Physiological Condition Dependent Changes in Ciliary GPCR Localization in the Brain.

MRAP2 regulates energy homeostasis by promoting primary cilia localization of MC4R.

KLF15 cistromes reveal a hepatocyte pathway governing plasma corticosteroid transport and systemic inflammation.

Melanocortin 4 receptor signals at the neuronal primary cilium to control food intake and body weight.

OR04-01 MRAP2 Regulates Energy Homeostasis by Promoting Primary Cilia Localization of MC4R.

Detailed 3-dimensional body shape features predict body composition, blood metabolites, and functional strength: the Shape Up! studies.

CRISPR-mediated activation of a promoter or enhancer rescues obesity caused by haploinsufficiency.

Genomic and epigenomic mapping of leptin-responsive neuronal populations involved in body weight regulation.

CRISPR-mediated activation of a promoter or enhancer rescues obesity caused by haploinsufficiency.

Subcellular localization of MC4R with ADCY3 at neuronal primary cilia underlies a common pathway for genetic predisposition to obesity.

Cilia and Obesity.

Acute Lesioning and Rapid Repair of Hypothalamic Neurons outside the Blood-Brain Barrier.

The Association of Serum Leptin with Mortality in Older Adults.

Genetic association study of adiposity and melanocortin-4 receptor (MC4R) common variants: replication and functional characterization of non-coding regions.

Hyperphagia: current concepts and future directions proceedings of the 2nd international conference on hyperphagia.

Functional characterization of SIM1-associated enhancers.

The melanocortin system and insulin resistance in humans: insights from a patient with complete POMC deficiency and type 1 diabetes mellitus.

Mechanism of N-terminal modulation of activity at the melanocortin-4 receptor GPCR.

Weight loss after Roux-en-Y gastric bypass in obese patients heterozygous for MC4R mutations.

Replication and extension of association between common genetic variants in SIM1 and human adiposity.

Monogenic Disorders Within the Energy Balance Pathway.

Changes in cortical bone response to high-fat diet from adolescence to adulthood in mice.

Systematic examination of the SIM1 gene region: Replication and extension of association between common genetic variants and adiposity.

Bariatric surgery in a patient with complete MC4R deficiency.

Reduced size-independent mechanical properties of cortical bone in high-fat diet-induced obesity.

In silico mutagenesis: a case study of the melanocortin 4 receptor.

Narrowing down the role of common variants in the genetic predisposition to obesity.

Identification, characterization and rescue of a novel vasopressin-2 receptor mutation causing nephrogenic diabetes insipidus.

Association of functionally significant Melanocortin-4 but not Melanocortin-3 receptor mutations with severe adult obesity in a large North American case-control study.

Unexpected endocrine features and normal pigmentation in a young adult patient carrying a novel homozygous mutation in the POMC gene.

Lessons from extreme human obesity: monogenic disorders.

Mutational analysis of the pro-opiomelanocortin gene in French obese children led to the identification of a novel deleterious heterozygous mutation located in the alpha-melanocyte stimulating hormone domain.

Gender and neurogenin3 influence the pathogenesis of ketosis-prone diabetes.

Engineering the melanocortin-4 receptor to control constitutive and ligand-mediated G(S) signaling in vivo.

Medical sequencing at the extremes of human body mass.

MUTATIONAL ANALYSIS OF THE PROOPIOMELANOCORTIN GENE IN OBESE CHILDREN.

Melanocortin 4 receptor mutations in a large cohort of severely obese adults: prevalence, functional classification, genotype-phenotype relationship, and lack of association with binge eating.

Obesity-associated mutations in the melanocortin 4 receptor provide novel insights into its function.

Lack of support for the association between GAD2 polymorphisms and severe human obesity.

High prevalence of glucose-6-phosphate dehydrogenase deficiency without gene mutation suggests a novel genetic mechanism predisposing to ketosis-prone diabetes.

Leptin regulation of bone resorption by the sympathetic nervous system and CART.

A statistical approach for array CGH data analysis.

PAX4 gene variations predispose to ketosis-prone diabetes.

Constitutive activity of the melanocortin-4 receptor is maintained by its N-terminal domain and plays a role in energy homeostasis in humans.

A homozygous null mutation delineates the role of the melanocortin-4 receptor in humans.

Ketosis-prone type 2 diabetes in patients of sub-Saharan African origin: clinical pathophysiology and natural history of beta-cell dysfunction and insulin resistance.

The human MC4R promoter: characterization and role in obesity.

Emerging trends in the search for genetic variants predisposing to human obesity.

Engineering the melanocortin-4 receptor to control G(s) signaling in vivo.

Molecular genetics of human obesity-associated MC4R mutations.

Intracellular retention is a common characteristic of childhood obesity-associated MC4R mutations.

Elevated plasma ghrelin levels in Prader Willi syndrome.

The human HNF-3 genes: cloning, partial sequence and mutation screening in patients with impaired glucose homeostasis.

Soluble leptin receptor in serum of subjects with complete resistance to leptin: relation to fat mass.

Melanocortin-4 receptor mutations are a frequent and heterogeneous cause of morbid obesity.

The Pro115Gln and Pro12Ala PPAR gamma gene mutations in obesity and type 2 diabetes.

Glycodelin: a pane in the implantation window.

Promegestone (R5020) and mifepristone (RU486) both function as progestational agonists of human glycodelin gene expression in isolated human epithelial cells.

A frameshift mutation in human MC4R is associated with a dominant form of obesity.

A mutation in the human leptin receptor gene causes obesity and pituitary dysfunction.

La mutation du gène du récepteur de la leptine entraîne chez l'homme une obésité massive associée à des anomalies hypothalamo-hypophysaires.

Pancreatic islet expression studies and polymorphic DNA markers in the genes encoding hepatocyte nuclear factor-3alpha, -3beta, -3gamma, -4gamma, and -6.

Leptin activation of Stat3 in the hypothalamus of wild-type and ob/ob mice but not db/db mice.

Gln-Arg192 polymorphism of paraoxonase and coronary heart disease in type 2 diabetes.

Genetic variation in the beta 3-adrenergic receptor and an increased capacity to gain weight in patients with morbid obesity.

A missense mutation in the glucagon receptor gene is associated with non-insulin-dependent diabetes mellitus.

Expression and regulation of adrenodoxin and P450scc mRNA in rodent tissues.

The human placental protein 14 (PP14) gene is localized on chromosome 9q34.

Human placental protein 14 gene: sequence and characterization of a short duplication.

cAMP regulates P450scc gene expression by a cycloheximide-insensitive mechanism in cultured mouse Leydig MA-10 cells.