Predominance of Null Mutations in Ataxia-Telangiectasia

Gilad, S; Khosravi, R; Shkedy, D; Uziel, T; Ziv, Y; Savitsky, K; Rotman, G; Smith, S; Chessa, L; Jorgensen, TJ; Harnik, R; Frydman, M; Sanal, O; Portnoi, S; Goldwicz, Z; Jaspers, NGJ; Gatti, RA; Lenoir, G; Lavin, MF; Tatsumi, K; Wegner, RD; Shiloh, Y; BarShira, A

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Tarih

1996

Yazar

Gilad, S

Khosravi, R

Shkedy, D

Uziel, T

Ziv, Y

Savitsky, K

Rotman, G

Smith, S

Chessa, L

Jorgensen, TJ

Harnik, R

Frydman, M

Sanal, O

Portnoi, S

Goldwicz, Z

Jaspers, NGJ

Gatti, RA

Lenoir, G

Lavin, MF

Tatsumi, K

Wegner, RD

Shiloh, Y

BarShira, A

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Özet

Ataxia-telangiectasia (A-T) is an autosomal recessive disorder involving cerebellar degeneration, immunodeficiency, chromosomal instability, radiosensitivity and cancer predisposition. The responsible gene, AIM, was recently identified by positional cloning and found to encode a putative 350 kDa protein with a PI 3-kinase-like domain, presumably involved in mediating cell cycle arrest in response to radiation-induced DNA damage. The nature and location of A-T mutations should provide insight into the function of the ATM protein and the molecular basis of this pleiotropic disease. Of 44 A-T mutations identified by us to date, 39 (89%) are expected to inactivate the ATM protein by truncating it, by abolishing correct initiation or termination of translation, or by deleting large segments. Additional mutations are four smaller in-frame deletions and insertions, and one substitution of a highly conserved amino acid at the PI 3-kinase domain. The emerging profile of mutations causing A-T is thus dominated by those expected to completely inactivate the AIM protein. ATM mutations with milder effects may result in phenotypes related, but not identical, to A-T.

Bağlantı

https://doi.org/10.1093/hmg/5.4.433
http://hdl.handle.net/11655/15270

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