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Homozygous defects in LMNA, encoding lamin A/C nuclear-envelope proteins, cause autosomal recessive axonal neuropathy in human (Charcot-Marie-Tooth disorder type 2) and mouse

  1. Author:
    De Sandre-Giovannoli, A.
    Chaouch, M.
    Kozlov, S.
    Vallat, J. M.
    Tazir, M.
    Kassouri, N.
    Szepetowski, P.
    Hammadouche, T.
    Vandenberghe, A.
    Stewart, C. L.
    Grid, D.
    Levy, N.

  2. Author Address

    Fac Med de la Timone, INSERM, U491, Unite Genet Med & Dev, F- 13385 Marseille 5, France. Fac Med de la Timone, INSERM, U491, Unite Genet Med & Dev, F-13385 Marseille 5, France. Hop Enfants La Timone, Dept Med Genet, Marseille, France. Inst Pasteur, Algiers, Algeria. NCI, Canc & Dev Biol Lab, Frederick, MD 21701 USA. Ctr Hosp Univ Dupuytren, Serv Neuropathol, Limoges, France. Hop Antiquaille, Neurogenet Lab, Lyon, France. Genethon 3, Evry, France. Levy N Fac Med de la Timone, INSERM, U491, Unite Genet Med & Dev, F-13385 Marseille 5, France.
    1. Year: 2002
  2. Journal: American Journal of Human Genetics
    1. 70
    2. 3
    3. Pages: 726-736
  4. Type of Article: Article
  1. Abstract:

    The Charcot-Marie-Tooth (CMT) disorders comprise a group of clinically and genetically heterogeneous hereditary motor and sensory neuropathies, which are mainly characterized by muscle weakness and wasting, foot deformities, and electrophysiological, as well as histological, changes. A subtype, CMT2, is defined by a slight or absent reduction of nerve-conduction velocities together with the loss of large myelinated fibers and axonal degeneration. CMT2 phenotypes are also characterized by a large genetic heterogeneity, although only two genes-NF-L and KIF1Bbeta-have been identified to date. Homozygosity mapping in inbred Algerian families with autosomal recessive CMT2 (AR-CMT2) provided evidence of linkage to chromosome 1q21.2-q21.3 in two families (Z(max) = 4.14). All patients shared a common homozygous ancestral haplotype that was suggestive of a founder mutation as the cause of the phenotype. A unique homozygous mutation in LMNA (which encodes lamin A/C, a component of the nuclear envelope) was identified in all affected members and in additional patients with CMT2 from a third, unrelated family. Ultrastructural exploration of sciatic nerves of LMNA null (i.e., -/-) mice was performed and revealed a strong reduction of axon density, axonal enlargement, and the presence of nonmyelinated axons, all of which were highly similar to the phenotypes of human peripheral axonopathies. The finding of site-specific amino acid substitutions in limb-girdle muscular dystrophy type 1B, autosomal dominant Emery-Dreifuss muscular dystrophy, dilated cardiomyopathy type 1A, autosomal dominant partial lipodystrophy, and, now, AR-CMT2 suggests the existence of distinct functional domains in lamin A/C that are essential for the maintenance and integrity of different cell lineages. To our knowledge, this report constitutes the first evidence of the recessive inheritance of a mutation that causes CMT2; additionally, we suggest that mutations in LMNA may also be the cause of the genetically overlapping disorder CMT2B1.

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