Compound Heterozygosity for Loss-of-Function Lysyl-tRNA Synthetase Mutations in a Patient with Peripheral Neuropathy | Zendy

Heather M. McLaughlin | Zendy; Reiko Sakaguchi | Zendy; Cuiping Liu | Zendy; Takao Igarashi | Zendy; Davut Pehli̇van | Zendy; Kristine Chu | Zendy; Ram Iyer | Zendy; Pedro Cruz | Zendy; Praveen F. Cherukuri | Zendy; Nancy F. Hansen | Zendy; James C. Mullikin | Zendy; Leslie G. Biesecker | Zendy; Thomas E. Wilson | Zendy; Victor Ionâşescu | Zendy; Garth A. Nicholson | Zendy; Charles Searby | Zendy; Kevin Talbot | Zendy; Jeffery M. Vance | Zendy; Stephan Züchner | Zendy; Kinga Szigeti | Zendy; James R. Lupski | Zendy; YaMing Hou | Zendy; Eric D. Green | Zendy; Anthony Antonellis | Zendy

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Compound Heterozygosity for Loss-of-Function Lysyl-tRNA Synthetase Mutations in a Patient with Peripheral Neuropathy

Author(s) -

Heather M. McLaughlin,

Reiko Sakaguchi,

Cuiping Liu,

Takao Igarashi,

Davut Pehli̇van,

Kristine Chu,

Ram Iyer,

Pedro Cruz,

Praveen F. Cherukuri,

Nancy F. Hansen,

James C. Mullikin,

Leslie G. Biesecker,

Thomas E. Wilson,

Victor Ionâşescu,

Garth A. Nicholson,

Charles Searby,

Kevin Talbot,

Jeffery M. Vance,

Stephan Züchner,

Kinga Szigeti,

James R. Lupski,

YaMing Hou,

Eric D. Green,

Anthony Antonellis

Publication year - 2010

Publication title -

the american journal of human genetics

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 6.661

H-Index - 302

eISSN - 1537-6605

pISSN - 0002-9297

DOI - 10.1016/j.ajhg.2010.09.008

Subject(s) - loss of heterozygosity , peripheral neuropathy , compound heterozygosity , transfer rna , peripheral , genetics , loss function , mutation , medicine , chemistry , microbiology and biotechnology , biochemistry , biology , endocrinology , phenotype , gene , rna , allele , diabetes mellitus

Charcot-Marie-Tooth (CMT) disease comprises a genetically and clinically heterogeneous group of peripheral nerve disorders characterized by impaired distal motor and sensory function. Mutations in three genes encoding aminoacyl-tRNA synthetases (ARSs) have been implicated in CMT disease primarily associated with an axonal pathology. ARSs are ubiquitously expressed, essential enzymes responsible for charging tRNA molecules with their cognate amino acids. To further explore the role of ARSs in CMT disease, we performed a large-scale mutation screen of the 37 human ARS genes in a cohort of 355 patients with a phenotype consistent with CMT. Here we describe three variants (p.Leu133His, p.Tyr173SerfsX7, and p.Ile302Met) in the lysyl-tRNA synthetase (KARS) gene in two patients from this cohort. Functional analyses revealed that two of these mutations (p.Leu133His and p.Tyr173SerfsX7) severely affect enzyme activity. Interestingly, both functional variants were found in a single patient with CMT disease and additional neurological and non-neurological sequelae. Based on these data, KARS becomes the fourth ARS gene associated with CMT disease, indicating that this family of enzymes is specifically critical for axon function.

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