James Gusella headshot

James Francis Gusella, Ph.D.

Bullard Professor of Neurogenetics in the Department of Genetics, Harvard Medical School
Research Staff, Massachusetts General Hospital

My laboratory is focused on understanding nervous system disease using molecular genetic strategies, beginning with human patients and proceeding through in vitro and modeling studies, with the ultimate goal of improving diagnosis, management and treatment.In any given disorder, the research can usually be divided into four sequential stages:

1. Determination of the chromosomal location of a gene defect, susceptibility gene or genetic modifier, usually based on linkage or association studies with polymorphic genetic markers.
2. Identification of the gene responsible for the phenotypic effect based upon its chromosomal location using a variety of genome analysis strategies.
3. Characterization of the mechanism of action based upon analysis of the allelic versions of the culprit gene in man, and in appropriate in vitro or in vivo model systems, including cultured human cells, genetically engineered mice, and lower organisms such as Drosophila and Dictyostelium.
4. Exploration of the potential for rational therapies, including genetic therapies.

We are currently searching for susceptibility and modifier genes in autism, Parkinson's disease, and Huntington's disease. As part of the Developmental Genome Anatomy Project, we also identify genes at breakpoints of balanced translocations associated with developmental abnormality. Finally we are examining the mechanism of pathogenesis of genetic defects in autism, biotin-responsive basal ganglia disease, Huntington's disease, Parkinson's disease, and neurofibromatosis, and pursuing assays to identify genetic and chemical modifiers, with the ultimate goal of contributing to effective rational therapies.

The NF2 gene and merlin protein in human osteosarcomas.
Authors: Authors: Stemmer-Rachamimov AO, Nielsen GP, Rosenberg AE, Louis DN, Jones D, Ramesh V, Gusella JF, Jacoby LB.
Neurogenetics
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Inflammatory bowel disease: is it in the genes?
Authors: Authors: Gusella JF, Podolsky DK.
Gastroenterology
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Huntingtin interacts with a family of WW domain proteins.
Authors: Authors: Faber PW, Barnes GT, Srinidhi J, Chen J, Gusella JF, MacDonald ME.
Hum Mol Genet
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The FERM domain: a unique module involved in the linkage of cytoplasmic proteins to the membrane.
Authors: Authors: Chishti AH, Kim AC, Marfatia SM, Lutchman M, Hanspal M, Jindal H, Liu SC, Low PS, Rouleau GA, Mohandas N, Chasis JA, Conboy JG, Gascard P, Takakuwa Y, Huang SC, Benz EJ, Bretscher A, Fehon RG, Gusella JF, Ramesh V, Solomon F, Marchesi VT, Tsukita S, Tsukita S, Hoover KB, et al.
Trends Biochem Sci
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Amyloid formation by mutant huntingtin: threshold, progressivity and recruitment of normal polyglutamine proteins.
Authors: Authors: Huang CC, Faber PW, Persichetti F, Mittal V, Vonsattel JP, MacDonald ME, Gusella JF.
Somat Cell Mol Genet
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Huntingtin: a single bait hooks many species.
Authors: Authors: Gusella JF, MacDonald ME.
Curr Opin Neurobiol
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Mice heterozygous for a mutation at the Nf2 tumor suppressor locus develop a range of highly metastatic tumors.
Authors: Authors: McClatchey AI, Saotome I, Mercer K, Crowley D, Gusella JF, Bronson RT, Jacks T.
Genes Dev
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Computer-mediated social support: single young mothers as a model system.
Authors: Authors: Dunham PJ, Hurshman A, Litwin E, Gusella J, Ellsworth C, Dodd PW.
Am J Community Psychol
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Molecular neurobiology and genetics: investigation of neural function and dysfunction.
Authors: Authors: Green T, Heinemann SF, Gusella JF.
Neuron
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Genetic variation in the 3' untranslated region of the neurofibromatosis 1 gene: application to unequal allelic expression.
Authors: Authors: Cowley GS, Murthy AE, Parry DM, Schneider G, Korf B, Upadhyaya M, Harper P, MacCollin M, Bernards A, Gusella JF.
Somat Cell Mol Genet
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