Abstract

This application proposes to support the career development of Alan H. Beggs, Ph.D., an Assistant Professor of Pediatrics at Children's Hospital and Harvard Medical School. The applicant's career goals are to continue developing a vigorous independent research program in muscle biology and human neuromuscular disease in the rich and stimulating environment of the Boston biomedical research community. Salary support via the KO2 mechanism will allow him to pursue full time research without having to perform a service function such as running a clinical diagnostic laboratory. The scientific goals of this proposal are to understand the structures, functions and protein interactions of muscle-specific alpha- actinins and to apply this information to the study of human neuromuscular disorders. The alpha-actinins are a family of closely related actin-binding proteins that serve to cross link and anchor actin filaments. In muscle, calcium-insensitive alpha-actinins are a major component of Z lines where they constitutively anchor the actin/nebulin-containing thin filaments. A number of human neuromuscular diseases have been shown to result from mutations of muscle-specific cytoskeletal elements. Similarly, several inherited cardiomyopathies are caused by mutations in genes for cardiac- specific isoforms of sarcomeric proteins. It is hypothesized that some human neuromuscular diseases may be caused by mutations in muscle-specific alpha-actinin genes, and/or in genes for proteins that interact with alpha-actinin. The applicant has cloned and characterized three genes for human o:-actinins and has recently identified several patients with congenital muscular dystrophy who lack expression of one of the muscle-specific isoforms. This proposal entails: l) extending this observation in additional patients with primary disorders of muscle and identifying mutations in the o(-actinin genes of deficient patients; 2) further characterizing (L-actinins in normal tissues; 3) developing cell culture and transgenic mouse models of alpha-actinin dysfunction; 4) identifying genes for novel proteins that interact with alpha- actinins; 5) characterizing these new genes and proteins: and 6) assessing these as candidate genes for other human neuromuscular diseases. Direct clinical benefits will include accurate pre- and postnatal diagnoses for these disorders, better understanding of their underlying etiology, and insights into potential therapies. These experiments will also increase our understanding of a-actinin function and identify new interactions with existing and novel muscle proteins at the Z-line and elsewhere.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Arthritis and Musculoskeletal and Skin Diseases (NIAMS)
Type
Research Scientist Development Award - Research (K02)
Project #
1K02AR002026-01
Application #
2005929
Study Section
Arthritis and Musculoskeletal and Skin Diseases Special Grants Review Committee (AMS)
Project Start
1997-06-23
Project End
2002-03-31
Budget Start
1997-06-23
Budget End
1998-03-31
Support Year
1
Fiscal Year
1997
Total Cost
Indirect Cost

  Institution

Name
Children's Hospital Boston
Department
Type
DUNS #
076593722
City
Boston
State
MA
Country
United States
Zip Code
02115

  Publications

Mizuno, Y; Puca, A A; O'Brien, K F et al. (2001) Genomic organization and single-nucleotide polymorphism map of desmuslin, a novel intermediate filament protein on chromosome 15q26.3. BMC Genet 2:8
Mills, M; Yang, N; Weinberger, R et al. (2001) Differential expression of the actin-binding proteins, alpha-actinin-2 and -3, in different species: implications for the evolution of functional redundancy. Hum Mol Genet 10:1335-46
Ryan, M M; Schnell, C; Strickland, C D et al. (2001) Nemaline myopathy: a clinical study of 143 cases. Ann Neurol 50:312-20
Takada, F; Vander Woude, D L; Tong, H Q et al. (2001) Myozenin: an alpha-actinin- and gamma-filamin-binding protein of skeletal muscle Z lines. Proc Natl Acad Sci U S A 98:1595-600
Gazda, H; Lipton, J M; Willig, T N et al. (2001) Evidence for linkage of familial Diamond-Blackfan anemia to chromosome 8p23.3-p22 and for non-19q non-8p disease. Blood 97:2145-50
Kaplan, J M; Kim, S H; North, K N et al. (2000) Mutations in ACTN4, encoding alpha-actinin-4, cause familial focal segmental glomerulosclerosis. Nat Genet 24:251-6
Wallgren-Pettersson, C; Pelin, K; Hilpela, P et al. (1999) Clinical and genetic heterogeneity in autosomal recessive nemaline myopathy. Neuromuscul Disord 9:564-72
North, K N; Yang, N; Wattanasirichaigoon, D et al. (1999) A common nonsense mutation results in alpha-actinin-3 deficiency in the general population. Nat Genet 21:353-4
Wattanasirichaigoon, D; Vesely, M R; Duggal, P et al. (1999) Sodium channel abnormalities are infrequent in patients with long QT syndrome: identification of two novel SCN5A mutations. Am J Med Genet 86:470-6
Satler, C A; Vesely, M R; Duggal, P et al. (1998) Multiple different missense mutations in the pore region of HERG in patients with long QT syndrome. Hum Genet 102:265-72

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