In-frame de novo mutation in BICD2 in two patients with muscular atrophy and arthrogryposis

Daniel C. Koboldt; Rama D. Kastury; Megan A. Waldrop; Benjamin J. Kelly; Theresa Mihalic Mosher; Heather McLaughlin; Don Corsmeier; Jonathan L. Slaughter; Kevin M. Flanigan; Kim L. McBride; Lakshmi Mehta; Richard K. Wilson; Peter White

doi:10.1101/mcs.a003160

In-frame de novo mutation in BICD2 in two patients with muscular atrophy and arthrogryposis

Daniel C. Koboldt
, Rama D. Kastury
, Megan A. Waldrop
, Benjamin J. Kelly
, Theresa Mihalic Mosher
, Heather McLaughlin
, Don Corsmeier
, Jonathan L. Slaughter
, Kevin M. Flanigan
, Kim L. McBride
, Lakshmi Mehta
, Richard K. Wilson
, Peter White

Icahn School of Medicine at Mount Sinai

Research output: Contribution to journal › Article › peer-review

18 Scopus citations

Abstract

We describe two unrelated patients, a 12-yr-old female and a 6-yr-old male, with congenital contractures and severe congenital muscular atrophy. Exome and genome sequencing of the probands and their unaffected parents revealed that they have the same de novo deletion in BICD2 (c.1636_1638delAAT). The variant, which has never been reported, results in an in-frame 3-bp deletion and is predicted to cause loss of an evolutionarily conserved asparagine residue at position 546 in the protein. Missense mutations in BICD2 cause autosomal dominant spinal muscular atrophy, lower-extremity predominant 2 (SMALED2), a disease characterized by muscle weakness and arthrogryposis of early onset and slow progression. The p.Asn546del clusters with four pathogenic missense variants in a region that likely binds molecular motor KIF5A. Protein modeling suggests that removing the highly conserved asparagine residue alters BICD2 protein structure. Our findings support a broader phenotypic spectrum of BICD2 mutations that may include severe manifestations such as cerebral atrophy, seizures, dysmorphic facial features, and profound muscular atrophy.

Original language	English
Journal	Cold Spring Harbor molecular case studies
Volume	4
Issue number	5
DOIs	https://doi.org/10.1101/mcs.a003160
State	Published - 1 Oct 2018

Keywords

absent speech
arthrogryposis multiplex congenita
decreased muscle mass
flexion contracture
fractures of the long bones
frontal bossing
generalized cerebral atrophy/hypoplasia
generalized muscle weakness
infantile spasms
prominent ear helix
relative macrocephaly
severe muscular hypotonia
skeletal myopathy
thick eyebrow

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10.1101/mcs.a003160

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Koboldt, D. C., Kastury, R. D., Waldrop, M. A., Kelly, B. J., Mosher, T. M., McLaughlin, H., Corsmeier, D., Slaughter, J. L., Flanigan, K. M., McBride, K. L., Mehta, L., Wilson, R. K., & White, P. (2018). In-frame de novo mutation in BICD2 in two patients with muscular atrophy and arthrogryposis. Cold Spring Harbor molecular case studies, 4(5). https://doi.org/10.1101/mcs.a003160

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title = "In-frame de novo mutation in BICD2 in two patients with muscular atrophy and arthrogryposis",

abstract = "We describe two unrelated patients, a 12-yr-old female and a 6-yr-old male, with congenital contractures and severe congenital muscular atrophy. Exome and genome sequencing of the probands and their unaffected parents revealed that they have the same de novo deletion in BICD2 (c.1636\_1638delAAT). The variant, which has never been reported, results in an in-frame 3-bp deletion and is predicted to cause loss of an evolutionarily conserved asparagine residue at position 546 in the protein. Missense mutations in BICD2 cause autosomal dominant spinal muscular atrophy, lower-extremity predominant 2 (SMALED2), a disease characterized by muscle weakness and arthrogryposis of early onset and slow progression. The p.Asn546del clusters with four pathogenic missense variants in a region that likely binds molecular motor KIF5A. Protein modeling suggests that removing the highly conserved asparagine residue alters BICD2 protein structure. Our findings support a broader phenotypic spectrum of BICD2 mutations that may include severe manifestations such as cerebral atrophy, seizures, dysmorphic facial features, and profound muscular atrophy.",

keywords = "absent speech, arthrogryposis multiplex congenita, decreased muscle mass, flexion contracture, fractures of the long bones, frontal bossing, generalized cerebral atrophy/hypoplasia, generalized muscle weakness, infantile spasms, prominent ear helix, relative macrocephaly, severe muscular hypotonia, skeletal myopathy, thick eyebrow",

author = "Koboldt, \{Daniel C.\} and Kastury, \{Rama D.\} and Waldrop, \{Megan A.\} and Kelly, \{Benjamin J.\} and Mosher, \{Theresa Mihalic\} and Heather McLaughlin and Don Corsmeier and Slaughter, \{Jonathan L.\} and Flanigan, \{Kevin M.\} and McBride, \{Kim L.\} and Lakshmi Mehta and Wilson, \{Richard K.\} and Peter White",

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year = "2018",

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doi = "10.1101/mcs.a003160",

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AU - Kastury, Rama D.

AU - Waldrop, Megan A.

AU - Kelly, Benjamin J.

AU - Mosher, Theresa Mihalic

AU - McLaughlin, Heather

AU - Corsmeier, Don

AU - Slaughter, Jonathan L.

AU - Flanigan, Kevin M.

AU - McBride, Kim L.

AU - Mehta, Lakshmi

AU - Wilson, Richard K.

AU - White, Peter

PY - 2018/10/1

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N2 - We describe two unrelated patients, a 12-yr-old female and a 6-yr-old male, with congenital contractures and severe congenital muscular atrophy. Exome and genome sequencing of the probands and their unaffected parents revealed that they have the same de novo deletion in BICD2 (c.1636_1638delAAT). The variant, which has never been reported, results in an in-frame 3-bp deletion and is predicted to cause loss of an evolutionarily conserved asparagine residue at position 546 in the protein. Missense mutations in BICD2 cause autosomal dominant spinal muscular atrophy, lower-extremity predominant 2 (SMALED2), a disease characterized by muscle weakness and arthrogryposis of early onset and slow progression. The p.Asn546del clusters with four pathogenic missense variants in a region that likely binds molecular motor KIF5A. Protein modeling suggests that removing the highly conserved asparagine residue alters BICD2 protein structure. Our findings support a broader phenotypic spectrum of BICD2 mutations that may include severe manifestations such as cerebral atrophy, seizures, dysmorphic facial features, and profound muscular atrophy.

AB - We describe two unrelated patients, a 12-yr-old female and a 6-yr-old male, with congenital contractures and severe congenital muscular atrophy. Exome and genome sequencing of the probands and their unaffected parents revealed that they have the same de novo deletion in BICD2 (c.1636_1638delAAT). The variant, which has never been reported, results in an in-frame 3-bp deletion and is predicted to cause loss of an evolutionarily conserved asparagine residue at position 546 in the protein. Missense mutations in BICD2 cause autosomal dominant spinal muscular atrophy, lower-extremity predominant 2 (SMALED2), a disease characterized by muscle weakness and arthrogryposis of early onset and slow progression. The p.Asn546del clusters with four pathogenic missense variants in a region that likely binds molecular motor KIF5A. Protein modeling suggests that removing the highly conserved asparagine residue alters BICD2 protein structure. Our findings support a broader phenotypic spectrum of BICD2 mutations that may include severe manifestations such as cerebral atrophy, seizures, dysmorphic facial features, and profound muscular atrophy.

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KW - arthrogryposis multiplex congenita

KW - decreased muscle mass

KW - flexion contracture

KW - fractures of the long bones

KW - frontal bossing

KW - generalized cerebral atrophy/hypoplasia

KW - generalized muscle weakness

KW - infantile spasms

KW - prominent ear helix

KW - relative macrocephaly

KW - severe muscular hypotonia

KW - skeletal myopathy

KW - thick eyebrow

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JO - Cold Spring Harbor molecular case studies

JF - Cold Spring Harbor molecular case studies

IS - 5

ER -

In-frame de novo mutation in BICD2 in two patients with muscular atrophy and arthrogryposis

Abstract

Keywords

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