Clinical and mutational spectrum of Colombian patients with Pelizaeus Merzbacher Disease

Parra Harvy Mauricio Velasco; Anaya Silvia Juliana Maradei; Guio Johanna Carolina Acosta; Diaz Clara Eugenia Arteaga; Rivera Juan Carlos Prieto

doi:10.25100/cm.v49i2.2522

Clinical and mutational spectrum of Colombian patients with Pelizaeus Merzbacher Disease

Parra Harvy Mauricio Velasco
, Anaya Silvia Juliana Maradei
, Guio Johanna Carolina Acosta
, Diaz Clara Eugenia Arteaga
, Rivera Juan Carlos Prieto

Institute of Human Genetics

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

4 Scopus citations

Abstract

Case Presentation: Pelizaeus Merzbacher Disease (PMD) is an X-linked developmental defect of myelination that causes childhood chronic spastic encephalopathy. Its genetic etiology can be either a duplication (or other gene dosage alterations) or a punctual mutation at the PLP1 locus. Clinically, it presents with developmental delay, nystagmus and, spasticity, supported by neuroimaging in which the defect of myelination is evident. We present a series of seven Colombian patients diagnosed with this leucodystrophy, describing their genotypic and phenotypic characteristics and heterogeneity. Clinical Findings: All patients included were male, 6 months to 16 years of age. Mean age at onset of symptoms was 8 months. Mean age at diagnosis was 5 years 5 months, being classic PMD most frequently diagnosed, as compared to the connatal phenotype. All cases had a primary diagnosis of developmental delay on 100%, and in 28.7% of cases, early onset nystagmus was described. 85.7% of patients had spasticity, 71.4% cerebellar signs, 57.0% hypotonia, and 28.5% had an abnormal movement disorder. Only three patients were able to achieve gait, though altered. In the two patients who had a diagnosis of connatal PMD maturational ages in danger zones according to the WHO Abbreviated Scale of Psychosocial Development were documented. All cases had abnormalities in neuroimages. Molecular Analysis and Results: Molecular studies were used in the majority of the cases to confirm the diagnosis (85.7%). For two cases molecular confirmation was not considered necessary given their affected male brothers had already been tested. PLP1 gene dosage alterations (duplications) were found in 28.5% of the patients (two siblings), whereas three different single nucleotide variants were detected. Clinical Relevance: According to these findings, as authors we propose the diagnostic algorithm in Colombian population to begin on a high clinical suspicion, followed by paraclinical extension, moving on to the molecular confirmation by using approaches to simultaneously sequence the PLP1 gene in order to detect point mutations and in/dels and performing a copy number variation analysis for the detection of gene dosage alterations.

Translated title of the contribution	Heterogeneidad clínica y mutacional en pacientes Colombianos con Pelizaeus Merzbacher
Original language	English
Pages (from-to)	182-187
Number of pages	6
Journal	Colombia Medica
Volume	49
Issue number	2
DOIs	https://doi.org/10.25100/cm.v49i2.2522
State	Published - 01 Apr 2018

Keywords

Child development
Developmental disorders
Myelin proteolipidic protein
Myelin sheath
PLP1
Pelizaeus merzbacherxs disease

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10.25100/cm.v49i2.2522

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title = "Clinical and mutational spectrum of Colombian patients with Pelizaeus Merzbacher Disease",

abstract = "Case Presentation: Pelizaeus Merzbacher Disease (PMD) is an X-linked developmental defect of myelination that causes childhood chronic spastic encephalopathy. Its genetic etiology can be either a duplication (or other gene dosage alterations) or a punctual mutation at the PLP1 locus. Clinically, it presents with developmental delay, nystagmus and, spasticity, supported by neuroimaging in which the defect of myelination is evident. We present a series of seven Colombian patients diagnosed with this leucodystrophy, describing their genotypic and phenotypic characteristics and heterogeneity. Clinical Findings: All patients included were male, 6 months to 16 years of age. Mean age at onset of symptoms was 8 months. Mean age at diagnosis was 5 years 5 months, being classic PMD most frequently diagnosed, as compared to the connatal phenotype. All cases had a primary diagnosis of developmental delay on 100\%, and in 28.7\% of cases, early onset nystagmus was described. 85.7\% of patients had spasticity, 71.4\% cerebellar signs, 57.0\% hypotonia, and 28.5\% had an abnormal movement disorder. Only three patients were able to achieve gait, though altered. In the two patients who had a diagnosis of connatal PMD maturational ages in danger zones according to the WHO Abbreviated Scale of Psychosocial Development were documented. All cases had abnormalities in neuroimages. Molecular Analysis and Results: Molecular studies were used in the majority of the cases to confirm the diagnosis (85.7\%). For two cases molecular confirmation was not considered necessary given their affected male brothers had already been tested. PLP1 gene dosage alterations (duplications) were found in 28.5\% of the patients (two siblings), whereas three different single nucleotide variants were detected. Clinical Relevance: According to these findings, as authors we propose the diagnostic algorithm in Colombian population to begin on a high clinical suspicion, followed by paraclinical extension, moving on to the molecular confirmation by using approaches to simultaneously sequence the PLP1 gene in order to detect point mutations and in/dels and performing a copy number variation analysis for the detection of gene dosage alterations.",

keywords = "Child development, Developmental disorders, Myelin proteolipidic protein, Myelin sheath, PLP1, Pelizaeus merzbacherxs disease",

author = "Velasco, \{Parra Harvy Mauricio\} and Maradei, \{Anaya Silvia Juliana\} and Acosta, \{Guio Johanna Carolina\} and Arteaga, \{Diaz Clara Eugenia\} and Prieto, \{Rivera Juan Carlos\}",

note = "Publisher Copyright: {\textcopyright} 2018 Universidad del Valle.",

year = "2018",

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doi = "10.25100/cm.v49i2.2522",

language = "English",

volume = "49",

pages = "182--187",

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T1 - Clinical and mutational spectrum of Colombian patients with Pelizaeus Merzbacher Disease

AU - Velasco, Parra Harvy Mauricio

AU - Maradei, Anaya Silvia Juliana

AU - Acosta, Guio Johanna Carolina

AU - Arteaga, Diaz Clara Eugenia

AU - Prieto, Rivera Juan Carlos

PY - 2018/4/1

Y1 - 2018/4/1

N2 - Case Presentation: Pelizaeus Merzbacher Disease (PMD) is an X-linked developmental defect of myelination that causes childhood chronic spastic encephalopathy. Its genetic etiology can be either a duplication (or other gene dosage alterations) or a punctual mutation at the PLP1 locus. Clinically, it presents with developmental delay, nystagmus and, spasticity, supported by neuroimaging in which the defect of myelination is evident. We present a series of seven Colombian patients diagnosed with this leucodystrophy, describing their genotypic and phenotypic characteristics and heterogeneity. Clinical Findings: All patients included were male, 6 months to 16 years of age. Mean age at onset of symptoms was 8 months. Mean age at diagnosis was 5 years 5 months, being classic PMD most frequently diagnosed, as compared to the connatal phenotype. All cases had a primary diagnosis of developmental delay on 100%, and in 28.7% of cases, early onset nystagmus was described. 85.7% of patients had spasticity, 71.4% cerebellar signs, 57.0% hypotonia, and 28.5% had an abnormal movement disorder. Only three patients were able to achieve gait, though altered. In the two patients who had a diagnosis of connatal PMD maturational ages in danger zones according to the WHO Abbreviated Scale of Psychosocial Development were documented. All cases had abnormalities in neuroimages. Molecular Analysis and Results: Molecular studies were used in the majority of the cases to confirm the diagnosis (85.7%). For two cases molecular confirmation was not considered necessary given their affected male brothers had already been tested. PLP1 gene dosage alterations (duplications) were found in 28.5% of the patients (two siblings), whereas three different single nucleotide variants were detected. Clinical Relevance: According to these findings, as authors we propose the diagnostic algorithm in Colombian population to begin on a high clinical suspicion, followed by paraclinical extension, moving on to the molecular confirmation by using approaches to simultaneously sequence the PLP1 gene in order to detect point mutations and in/dels and performing a copy number variation analysis for the detection of gene dosage alterations.

AB - Case Presentation: Pelizaeus Merzbacher Disease (PMD) is an X-linked developmental defect of myelination that causes childhood chronic spastic encephalopathy. Its genetic etiology can be either a duplication (or other gene dosage alterations) or a punctual mutation at the PLP1 locus. Clinically, it presents with developmental delay, nystagmus and, spasticity, supported by neuroimaging in which the defect of myelination is evident. We present a series of seven Colombian patients diagnosed with this leucodystrophy, describing their genotypic and phenotypic characteristics and heterogeneity. Clinical Findings: All patients included were male, 6 months to 16 years of age. Mean age at onset of symptoms was 8 months. Mean age at diagnosis was 5 years 5 months, being classic PMD most frequently diagnosed, as compared to the connatal phenotype. All cases had a primary diagnosis of developmental delay on 100%, and in 28.7% of cases, early onset nystagmus was described. 85.7% of patients had spasticity, 71.4% cerebellar signs, 57.0% hypotonia, and 28.5% had an abnormal movement disorder. Only three patients were able to achieve gait, though altered. In the two patients who had a diagnosis of connatal PMD maturational ages in danger zones according to the WHO Abbreviated Scale of Psychosocial Development were documented. All cases had abnormalities in neuroimages. Molecular Analysis and Results: Molecular studies were used in the majority of the cases to confirm the diagnosis (85.7%). For two cases molecular confirmation was not considered necessary given their affected male brothers had already been tested. PLP1 gene dosage alterations (duplications) were found in 28.5% of the patients (two siblings), whereas three different single nucleotide variants were detected. Clinical Relevance: According to these findings, as authors we propose the diagnostic algorithm in Colombian population to begin on a high clinical suspicion, followed by paraclinical extension, moving on to the molecular confirmation by using approaches to simultaneously sequence the PLP1 gene in order to detect point mutations and in/dels and performing a copy number variation analysis for the detection of gene dosage alterations.

KW - Child development

KW - Developmental disorders

KW - Myelin proteolipidic protein

KW - Myelin sheath

KW - PLP1

KW - Pelizaeus merzbacherxs disease

UR - https://www.scopus.com/pages/publications/85051434139

U2 - 10.25100/cm.v49i2.2522

DO - 10.25100/cm.v49i2.2522

M3 - Article

C2 - 30104812

AN - SCOPUS:85051434139

SN - 0120-8322

VL - 49

SP - 182

EP - 187

JO - Colombia Medica

JF - Colombia Medica

IS - 2

ER -

Clinical and mutational spectrum of Colombian patients with Pelizaeus Merzbacher Disease

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Keywords

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