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Literature DB >> 19369543

Connexin32 mutations cause loss of function in Schwann cells and oligodendrocytes leading to PNS and CNS myelination defects.

Irene Sargiannidou¹, Natalie Vavlitou, Sophia Aristodemou, Andreas Hadjisavvas, Kyriacos Kyriacou, Steven S Scherer, Kleopas A Kleopa.

Abstract

The gap junction (GJ) protein connexin32 (Cx32) is expressed by myelinating Schwann cells and oligodendrocytes and is mutated in X-linked Charcot-Marie-Tooth disease. In addition to a demyelinating peripheral neuropathy, some Cx32 mutants are associated with transient or chronic CNS phenotypes. To investigate the molecular basis of these phenotypes, we generated transgenic mice expressing the T55I or the R75W mutation and an IRES-EGFP, driven by the mouse Cnp promoter. The transgene was expressed in oligodendrocytes throughout the CNS and in Schwann cells. Both the T55I and the R75W mutants were localized in the perinuclear cytoplasm, did not form GJ plaques, and did not alter the expression or localization of two other oligodendrocytic GJ proteins, Cx47 and Cx29, or the expression of Cx29 in Schwann cells. On wild type background, the expression of endogenous mCx32 was unaffected by the T55I mutant, but was partly impaired by R75W. Transgenic mice with the R75W mutation and all mutant animals with Gjb1-null background developed a progressive demyelinating peripheral neuropathy along with CNS myelination defects. These findings suggest that Cx32 mutations result in loss of function in myelinated cells without trans-dominant effects on other GJ proteins. Loss of Cx32 function alone in the CNS causes myelination defects.

Entities: Chemical Disease Gene Mutation Species

Mesh：

Substances：
Connexins
connexin 32

Year: 2009 PMID： 19369543 PMCID： PMC2721059 DOI： 10.1523/JNEUROSCI.0325-09.2009

Source DB: PubMed Journal: J Neurosci ISSN： 0270-6474 Impact factor: 6.167

62 in total

1. The CNS phenotype of X-linked Charcot-Marie-Tooth disease: more than a peripheral problem.

Authors: Robert A Taylor; Erin M Simon; Harold G Marks; Steven S Scherer
Journal: Neurology Date: 2003-12-09 Impact factor: 9.910

2. Genetic and physiological evidence that oligodendrocyte gap junctions contribute to spatial buffering of potassium released during neuronal activity.

Authors: Daniela M Menichella; Marta Majdan; Rajeshwar Awatramani; Daniel A Goodenough; Erich Sirkowski; Steven S Scherer; David L Paul
Journal: J Neurosci Date: 2006-10-25 Impact factor: 6.167

Review 3. Molecular genetics of X-linked Charcot-Marie-Tooth disease.

Authors: Kleopas A Kleopa; Steven S Scherer
Journal: Neuromolecular Med Date: 2006 Impact factor: 3.843

4. CMT1X phenotypes represent loss of GJB1 gene function.

Authors: M E Shy; C Siskind; E R Swan; K M Krajewski; T Doherty; D R Fuerst; P J Ainsworth; R A Lewis; S S Scherer; A F Hahn
Journal: Neurology Date: 2007-03-13 Impact factor: 9.910

5. GJA12 mutations in children with recessive hypomyelinating leukoencephalopathy.

Authors: M Bugiani; S Al Shahwan; E Lamantea; A Bizzi; E Bakhsh; I Moroni; M R Balestrini; G Uziel; M Zeviani
Journal: Neurology Date: 2006-05-17 Impact factor: 9.910

6. The inner ear contains heteromeric channels composed of cx26 and cx30 and deafness-related mutations in cx26 have a dominant negative effect on cx30.

Authors: Andrew Forge; Nerissa K Marziano; Stefano O Casalotti; David L Becker; Daniel Jagger
Journal: Cell Commun Adhes Date: 2003 Jul-Dec

7. Connexins are critical for normal myelination in the CNS.

Authors: Daniela M Menichella; Daniel A Goodenough; Erich Sirkowski; Steven S Scherer; David L Paul
Journal: J Neurosci Date: 2003-07-02 Impact factor: 6.167

8. Coupling of astrocyte connexins Cx26, Cx30, Cx43 to oligodendrocyte Cx29, Cx32, Cx47: Implications from normal and connexin32 knockout mice.

Authors: J I Nagy; A-V Ionescu; B D Lynn; J E Rash
Journal: Glia Date: 2003-12 Impact factor: 7.452

9. Molecular interaction of connexin 30.3 and connexin 31 suggests a dominant-negative mechanism associated with erythrokeratodermia variabilis.

Authors: Laure Plantard; Marcel Huber; Francoise Macari; Paolo Meda; Daniel Hohl
Journal: Hum Mol Genet Date: 2003-10-28 Impact factor: 6.150

10. Loss-of-function GJA12/Connexin47 mutations cause Pelizaeus-Merzbacher-like disease.

Authors: Jennifer L Orthmann-Murphy; Alan D Enriquez; Charles K Abrams; Steven S Scherer
Journal: Mol Cell Neurosci Date: 2007-01-25 Impact factor: 4.314

41 in total

1. The role of gap junctions in Charcot-Marie-Tooth disease.

Authors: Kleopas A Kleopa
Journal: J Neurosci Date: 2011-12-07 Impact factor: 6.167

2. Inflammatory demyelinating CNS disorder in a case of X-linked Charcot-Marie-Tooth disease: positive response to natalizumab.

Authors: Jochen H Weishaupt; Claudia Ganser; Mathias Bähr
Journal: J Neurol Date: 2012-03-13 Impact factor: 4.849

Review 3. Brain connexins in demyelinating diseases: therapeutic potential of glial targets.

Authors: Maria Luisa Cotrina; Maiken Nedergaard
Journal: Brain Res Date: 2012-07-10 Impact factor: 3.252

4. Axonal pathology precedes demyelination in a mouse model of X-linked demyelinating/type I Charcot-Marie Tooth neuropathy.

Authors: Natalie Vavlitou; Irene Sargiannidou; Kyriaki Markoullis; Kyriacos Kyriacou; Steven S Scherer; Kleopas A Kleopa
Journal: J Neuropathol Exp Neurol Date: 2010-09 Impact factor: 3.685

5. Selective Cre-mediated gene deletion identifies connexin 43 as the main connexin channel supporting olfactory ensheathing cell networks.

Authors: Ana Paula Piantanida; Luis Ernesto Acosta; Lucila Brocardo; Claudia Capurro; Charles A Greer; Lorena Rela
Journal: J Comp Neurol Date: 2019-01-21 Impact factor: 3.215