Molecular Defects in the Motor Adaptor BICD2 Cause Proximal Spinal Muscular Atrophy with Autosomal-Dominant Inheritance

Peeters, Kris; Litvinenko, Ivan; Asselbergh, Bob; Almeida-Souza, Le­onardo; Chamova, Teodora; Geuens, Thomas; Ydens, Elke; Zimoń, M.; Irobi, Joy; Vriendt, Els De; Winter, Vicky De; Ooms, Tinne; Timmerman, Vincent; Tournev, Ivailo; Jordanova, Albena

doi:10.1016/j.ajhg.2013.04.013

Cited by 118 publications

(127 citation statements)

References 38 publications

(56 reference statements)

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“…Studies in rodents have shown that this protein plays an important role in dynein-based cargo transport in neurons (32)(33)(34). Consistent with these findings, missense mutations in the human BICD2 gene are also associated with SMALED (35)(36)(37) and cortical malformations (38,39). The protein uses an N-terminal coiled-coil domain (BICD2N) to bind dynein and dynactin and a C-terminal coiled coil (BICD2C) to bind cargos (17).…”

Section: Significancesupporting

confidence: 49%

DYNC1H1 mutations associated with neurological diseases compromise processivity of dynein–dynactin–cargo adaptor complexes

Hoang

Schlager

Carter

et al. 2017

Proc. Natl. Acad. Sci. U.S.A.

104

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Mutations in the human DYNC1H1 gene are associated with neurological diseases. DYNC1H1 encodes the heavy chain of cytoplasmic dynein-1, a 1.4-MDa motor complex that traffics organelles, vesicles, and macromolecules toward microtubule minus ends. The effects of the DYNC1H1 mutations on dynein motility, and consequently their links to neuropathology, are not understood. Here, we address this issue using a recombinant expression system for human dynein coupled to single-molecule resolution in vitro motility assays. We functionally characterize 14 DYNC1H1 mutations identified in humans diagnosed with malformations in cortical development (MCD) or spinal muscular atrophy with lower extremity predominance (SMALED), as well as three mutations that cause motor and sensory defects in mice. Two of the human mutations, R1962C and H3822P, strongly interfere with dynein's core mechanochemical properties. The remaining mutations selectively compromise the processive mode of dynein movement that is activated by binding to the accessory complex dynactin and the cargo adaptor Bicaudal-D2 (BICD2). Mutations with the strongest effects on dynein motility in vitro are associated with MCD. The vast majority of mutations do not affect binding of dynein to dynactin and BICD2 and are therefore expected to result in linkage of cargos to dynein-dynactin complexes that have defective long-range motility. This observation offers an explanation for the dominant effects of DYNC1H1 mutations in vivo. Collectively, our results suggest that compromised processivity of cargo-motor assemblies contributes to human neurological disease and provide insight into the influence of different regions of the heavy chain on dynein motility. dynein | DYNC1H1 | neurological disease | cargo adaptor | processivity

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Section: Significancesupporting

confidence: 49%

DYNC1H1 mutations associated with neurological diseases compromise processivity of dynein–dynactin–cargo adaptor complexes

Hoang

Schlager

Carter

et al. 2017

Proc. Natl. Acad. Sci. U.S.A.

104

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“…1 Recently, BICD2 has been identified to cause dominant SMA. [1][2][3] Here, we provide additional evidence that BICD2 is a cause of dominant SMA and report detailed clinical, electrophysiological and MRI data from a three-generation family with cosegregation of a novel BICD2 mutation. These findings extend current notions of BICD2, demonstrating that it can present with adult-onset combined proximal and distal lower extremity SMA.…”

mentioning

confidence: 89%

Dominant spinal muscular atrophy due to BICD2: a novel mutation refines the phenotype

Synofzik

Martinez-Carrera

Lindig

et al. 2013

Journal of Neurology, Neurosurgery & Psychiatry

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“…These patients are characterized by non-progressive congenital or earlyonset lower-limb-predominant weakness, which often results in significant mobility impairment. Secondly, Peeters et al [68] found mutations in BICD2 in independent Bulgarian families with autosomal-dominant proximal SMA. First, Oates et al [67] reported several missense mutations in BICD2 in patients affected with DCSMA or DCSMA with upper motor neuron features, or HSP (hereditary spastic paraplegia).…”

Section: Mutations In Bicd2mentioning

confidence: 99%

“…Secondly, Peeters et al [68] found mutations in BICD2 in independent Bulgarian families with autosomal-dominant proximal SMA. Some experimental evidence exists: BICD2-R501P and BICD2-S107L mutants increase dynein-dynactin binding and the BICD2-Q774G mutant decreases Rab6 binding [67,68]. Thirdly, Neveling et al [69] described four BICD2 mutations in Dutch and Canadian families afflicted with autosomal-dominant SMA, with weakness and atrophy of proximal and distal muscles mainly of the legs.…”

Section: Mutations In Bicd2mentioning

confidence: 99%

Mutations in cytoplasmic dynein and its regulators cause malformations of cortical development and neurodegenerative diseases

Lipka

Kuijpers

Jaworski

et al. 2013

Biochemical Society Transactions

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Neurons are highly specialized for the processing and transmission of electrical signals and use cytoskeleton-based motor proteins to transport different vesicles and cellular materials. Abnormalities in intracellular transport are thought to be a critical factor in the degeneration and death of neurons in both the central and peripheral nervous systems. Several recent studies describe disruptive mutations in the minus-end-directed microtubule motor cytoplasmic dynein that are directly linked to human motor neuropathies, such as SMA (spinal muscular atrophy) and axonal CMT (Charcot-Marie-Tooth) disease or malformations of cortical development, including lissencephaly, pachygyria and polymicrogyria. In addition, genetic defects associated with these and other neurological disorders have been found in multifunctional adaptors that regulate dynein function, including the dynactin subunit p150(Glued), BICD2 (Bicaudal D2), Lis-1 (lissencephaly 1) and NDE1 (nuclear distribution protein E). In the present paper we provide an overview of the disease-causing mutations in dynein motors and regulatory proteins that lead to a broad phenotypic spectrum extending from peripheral neuropathies to cerebral malformations.

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Molecular Defects in the Motor Adaptor BICD2 Cause Proximal Spinal Muscular Atrophy with Autosomal-Dominant Inheritance

Cited by 118 publications

References 38 publications

DYNC1H1 mutations associated with neurological diseases compromise processivity of dynein–dynactin–cargo adaptor complexes

DYNC1H1 mutations associated with neurological diseases compromise processivity of dynein–dynactin–cargo adaptor complexes

Dominant spinal muscular atrophy due to BICD2: a novel mutation refines the phenotype

Mutations in cytoplasmic dynein and its regulators cause malformations of cortical development and neurodegenerative diseases

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