Expanding the ADCY5 phenotype toward spastic paraparesis : Amutation in the M2 domain

Waalkens, Anne J.E.; Vansenne, Fleur; Van Der Hout, Annemarie H.; Zutt, Rodi; Mourmans, Jeroen; Tolosa, Eduardo; De Koning, Tom J.; Tijssen, Marina A.J.

Expanding the ADCY5 phenotype toward spastic paraparesis : Amutation in the M2 domain

Mark

Waalkens, Anne J.E. ; Vansenne, Fleur ; Van Der Hout, Annemarie H. ; Zutt, Rodi ; Mourmans, Jeroen ; Tolosa, Eduardo ; De Koning, Tom J. ^LU and Tijssen, Marina A.J. (2018) In Neurology: Genetics 4(1).

Abstract: Patients with an ADCY5 gene mutation reveal a heterogenous clinical presentation including axial hypotonia, motor milestone delay, fluctuating dyskinesias, dystonia, and/or myoclonus with episodic exacerbations during drowsiness and sleep.^1,2 Phenotype-genotype correlations and somatic mosaicism are suggested to explain the wide phenotypic spectrum.¹ The ADCY5 gene encodes 1 of 9 membrane-bound adenyl cyclases converting adenosine triphosphate to cyclic adenosine-39, 59-monophosphate, the second messenger in a range of cellular activities.³ The ADCY5 protein contains 2 transmembrane domains, M1 and M2, and 2 bipartite cytoplasmic domains, C1 and C2. Pathogenic mutations have been described in domains C1... (More); Patients with an ADCY5 gene mutation reveal a heterogenous clinical presentation including axial hypotonia, motor milestone delay, fluctuating dyskinesias, dystonia, and/or myoclonus with episodic exacerbations during drowsiness and sleep.^1,2 Phenotype-genotype correlations and somatic mosaicism are suggested to explain the wide phenotypic spectrum.¹ The ADCY5 gene encodes 1 of 9 membrane-bound adenyl cyclases converting adenosine triphosphate to cyclic adenosine-39, 59-monophosphate, the second messenger in a range of cellular activities.³ The ADCY5 protein contains 2 transmembrane domains, M1 and M2, and 2 bipartite cytoplasmic domains, C1 and C2. Pathogenic mutations have been described in domains C1 and C2.^1,2 Mutations are likely to have a gain-of-function effect based on increased cyclic adenosine-39, 59-monophosphate accumulation.⁴ The present report describes 3 cases of ADCY5 dyskinesia to further illustrate the clinical spectrum: a new phenotype, i.e., spastic paraparesis due to a mutation located in the M2 domain; case 1, case 2, and case 3 show previously described mutations in the C1 domain of the ADCY5 protein. Their phenotypes show important similarities to previous cases, with the addition of the psychiatric symptoms of the patient in case 3.
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Please use this url to cite or link to this publication: https://lup.lub.lu.se/record/a44d1ee8-d083-4e28-8d6a-f03b244a3648

author

Waalkens, Anne J.E. ; Vansenne, Fleur ; Van Der Hout, Annemarie H. ; Zutt, Rodi ; Mourmans, Jeroen ; Tolosa, Eduardo ; De Koning, Tom J. ^LU and Tijssen, Marina A.J.

publishing date

2018-02

type

Contribution to journal

publication status

published

subject

in

Neurology: Genetics

volume

4

issue

1

article number

e214

publisher

Lippincott Williams & Wilkins

external identifiers

scopus:85048702231

ISSN

2376-7839

DOI

10.1212/NXG.0000000000000214

language

English

LU publication?

no

id

a44d1ee8-d083-4e28-8d6a-f03b244a3648

date added to LUP

2020-02-11 12:40:05

date last changed

2022-04-18 20:47:19

@article{a44d1ee8-d083-4e28-8d6a-f03b244a3648,
  abstract     = {{<p>Patients with an ADCY5 gene mutation reveal a heterogenous clinical presentation including axial hypotonia, motor milestone delay, fluctuating dyskinesias, dystonia, and/or myoclonus with episodic exacerbations during drowsiness and sleep.<sup>1,2</sup> Phenotype-genotype correlations and somatic mosaicism are suggested to explain the wide phenotypic spectrum.<sup>1</sup> The ADCY5 gene encodes 1 of 9 membrane-bound adenyl cyclases converting adenosine triphosphate to cyclic adenosine-39, 59-monophosphate, the second messenger in a range of cellular activities.<sup>3</sup> The ADCY5 protein contains 2 transmembrane domains, M1 and M2, and 2 bipartite cytoplasmic domains, C1 and C2. Pathogenic mutations have been described in domains C1 and C2.<sup>1,2</sup> Mutations are likely to have a gain-of-function effect based on increased cyclic adenosine-39, 59-monophosphate accumulation.<sup>4</sup> The present report describes 3 cases of ADCY5 dyskinesia to further illustrate the clinical spectrum: a new phenotype, i.e., spastic paraparesis due to a mutation located in the M2 domain; case 1, case 2, and case 3 show previously described mutations in the C1 domain of the ADCY5 protein. Their phenotypes show important similarities to previous cases, with the addition of the psychiatric symptoms of the patient in case 3.</p>}},
  author       = {{Waalkens, Anne J.E. and Vansenne, Fleur and Van Der Hout, Annemarie H. and Zutt, Rodi and Mourmans, Jeroen and Tolosa, Eduardo and De Koning, Tom J. and Tijssen, Marina A.J.}},
  issn         = {{2376-7839}},
  language     = {{eng}},
  number       = {{1}},
  publisher    = {{Lippincott Williams & Wilkins}},
  series       = {{Neurology: Genetics}},
  title        = {{Expanding the ADCY5 phenotype toward spastic paraparesis : Amutation in the M2 domain}},
  url          = {{http://dx.doi.org/10.1212/NXG.0000000000000214}},
  doi          = {{10.1212/NXG.0000000000000214}},
  volume       = {{4}},
  year         = {{2018}},
}

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Expanding the ADCY5 phenotype toward spastic paraparesis : Amutation in the M2 domain