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The genetic landscape of axonal neuropathies in the middle-aged and elderly: Focus on MME

. 2020 Dec 15 ; 95 (24) : e3163-e3179. [epub] 20201103

Language English Country United States Media print-electronic

Document type Journal Article, Research Support, N.I.H., Extramural, Research Support, Non-U.S. Gov't

Persistent link   https://www.medvik.cz/link/pmid33144514

Grant support
MR/N025431/1 Medical Research Council - United Kingdom
MR/N010035/1 Medical Research Council - United Kingdom
G1000848 Medical Research Council - United Kingdom
U54 NS065712 NINDS NIH HHS - United States
MR/N025431/2 Medical Research Council - United Kingdom
R01 NS075764 NINDS NIH HHS - United States
U01 HG010218 NHGRI NIH HHS - United States
MR/N027302/1 Medical Research Council - United Kingdom
I 4699 Austrian Science Fund FWF - Austria
U01 HG007708 NHGRI NIH HHS - United States

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PubMed 33144514
PubMed Central PMC7836667
DOI 10.1212/wnl.0000000000011132
PII: WNL.0000000000011132
Knihovny.cz E-resources

OBJECTIVE: To test the hypothesis that monogenic neuropathies such as Charcot-Marie-Tooth disease (CMT) contribute to frequent but often unexplained neuropathies in the elderly, we performed genetic analysis of 230 patients with unexplained axonal neuropathies and disease onset ≥35 years. METHODS: We recruited patients, collected clinical data, and conducted whole-exome sequencing (WES; n = 126) and MME single-gene sequencing (n = 104). We further queried WES repositories for MME variants and measured blood levels of the MME-encoded protein neprilysin. RESULTS: In the WES cohort, the overall detection rate for assumed disease-causing variants in genes for CMT or other conditions associated with neuropathies was 18.3% (familial cases 26.4%, apparently sporadic cases 12.3%). MME was most frequently involved and accounted for 34.8% of genetically solved cases. The relevance of MME for late-onset neuropathies was further supported by detection of a comparable proportion of cases in an independent patient sample, preponderance of MME variants among patients compared to population frequencies, retrieval of additional late-onset neuropathy patients with MME variants from WES repositories, and low neprilysin levels in patients' blood samples. Transmission of MME variants was often consistent with an incompletely penetrant autosomal-dominant trait and less frequently with autosomal-recessive inheritance. CONCLUSIONS: A detectable fraction of unexplained late-onset axonal neuropathies is genetically determined, by variants in either CMT genes or genes involved in other conditions that affect the peripheral nerves and can mimic a CMT phenotype. MME variants can act as completely penetrant recessive alleles but also confer dominantly inherited susceptibility to axonal neuropathies in an aging population.

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