Case Report: Contiguous Xq22.3 Deletion Associated with ATS-ID
Syndrome: From Genotype to Further Delineation of the Phenotype

J 2021

Case Report: Contiguous Xq22.3 Deletion Associated with ATS-ID Syndrome: From Genotype to Further Delineation of the Phenotype

SMETANA, Jan; Vladimíra VALLOVÁ; Markéta WAYHELOVÁ; Eva HLADÍLKOVÁ; Hana FILKOVÁ et al.

Základní údaje

Originální název

Case Report: Contiguous Xq22.3 Deletion Associated with ATS-ID Syndrome: From Genotype to Further Delineation of the Phenotype

Autoři

SMETANA, Jan; Vladimíra VALLOVÁ; Markéta WAYHELOVÁ; Eva HLADÍLKOVÁ; Hana FILKOVÁ; Věra HOŘÍNOVÁ; Petr BROŽ; Aneta MIKULÁŠOVÁ; Renata GAILLYOVÁ a Petr KUGLÍK

Vydání

Frontiers in Genetics, Frontiers Media S.A. 2021, 1664-8021

Další údaje

Jazyk

angličtina

Typ výsledku

Článek v odborném periodiku

Obor

10603 Genetics and heredity

Stát vydavatele

Švýcarsko

Utajení

není předmětem státního či obchodního tajemství

Odkazy

URL

Impakt faktor

Impact factor: 4.772

Označené pro přenos do RIV

Ano

Kód RIV

RIV/00216224:14310/21:00120159

Organizační jednotka

Přírodovědecká fakulta

Klíčová slova anglicky

ATS-MR syndrome; trio-based whole exome sequencing; genotype-phenotype analysis; neurodevelopmental disorders; Xq22.3q23 deletions

Štítky

14314010, rivok

Příznaky

Mezinárodní význam, Recenzováno

Změněno: 24. 11. 2021 10:42, Mgr. Marie Novosadová Šípková, DiS.

Anotace

V originále

Alport syndrome with intellectual disability (ATS-ID, AMME complex; OMIM #300194) is an X-linked contiguous gene deletion syndrome associated with an Xq22.3 locus mainly characterized by hematuria, renal failure, hearing loss/deafness, neurodevelopmental disorder (NDD), midface retrusion, and elliptocytosis. It is thought that ATS-ID is caused by the loss of function of COL4A5 (ATS) and FACL4 (ACSL4) genes through the interstitial (micro)deletion of chromosomal band Xq22.3. We report detailed phenotypic description and results from genome-wide screening of a Czech family with diagnosis ATS-ID (proband, maternal uncle, and two female carriers). Female carriers showed mild clinical features of microscopic hematuria only, while affected males displayed several novel clinical features associated with ATS-ID. Utilization of whole-exome sequencing discovered the presence of approximately 3 Mb of deletion in the Xq23 area, which affected 19 genes from TSC22D3 to CHRDL1. We compared the clinical phenotype with previously reported three ATS-ID families worldwide and correlated their clinical manifestations with the incidence of genes in both telomeric and centromeric regions of the deleted chromosomal area. In addition to previously described phenotypes associated with aberrations in AMMECR1 and FACL4, we identified two genes, members of tripartite motif family MID2 and subunit of the proteasome PA700/19S complex (PSMD10), respectively, as prime candidate genes responsible for additional clinical features observed in our patients with ATS-ID. Overall, our findings further improve the knowledge about the clinical impact of Xq23 deletions and bring novel information about phenotype/genotype association of this chromosomal aberration.

Návaznosti

NU20-07-00145, projekt VaV

Název: Úloha patogenních genetických variant detekovaných pomocí exomového sekvenování v etiologii dětských neurovývojových onemocnění

Investor: Ministerstvo zdravotnictví ČR, Úloha patogenních genetických variant detekovaných pomocí exomového sekvenování v etiologii dětských neurovývojových onemocnění, Podprogram 1 - standardní

Citovat

SMETANA, Jan; Vladimíra VALLOVÁ; Markéta WAYHELOVÁ; Eva HLADÍLKOVÁ; Hana FILKOVÁ; Věra HOŘÍNOVÁ; Petr BROŽ; Aneta MIKULÁŠOVÁ; Renata GAILLYOVÁ a Petr KUGLÍK. Case Report: Contiguous Xq22.3 Deletion Associated with ATS-ID Syndrome: From Genotype to Further Delineation of the Phenotype. Frontiers in Genetics. Frontiers Media S.A., 2021, roč. 12, October, s. 750110-750116. ISSN 1664-8021. Dostupné z: https://doi.org/10.3389/fgene.2021.750110.

@article{1800799,
   author = {Smetana, Jan and Vallová, Vladimíra and Wayhelová, Markéta and Hladílková, Eva and Filková, Hana and Hořínová, Věra and Brož, Petr and Mikulášová, Aneta and Gaillyová, Renata and Kuglík, Petr},
   article_number = {October},
   doi = {https://doi.org/10.3389/fgene.2021.750110},
   keywords = {ATS-MR syndrome; trio-based whole exome sequencing; genotype-phenotype analysis; neurodevelopmental disorders; Xq22.3q23 deletions},
   language = {eng},
   issn = {1664-8021},
   journal = {Frontiers in Genetics},
   title = {Case Report: Contiguous Xq22.3 Deletion Associated with ATS-ID Syndrome: From Genotype to Further Delineation of the Phenotype},
   url = {https://doi.org/10.3389/fgene.2021.750110},
   volume = {12},
   year = {2021}
}

TY  - JOUR
ID  - 1800799
AU  - Smetana, Jan - Vallová, Vladimíra - Wayhelová, Markéta - Hladílková, Eva - Filková, Hana - Hořínová, Věra - Brož, Petr - Mikulášová, Aneta - Gaillyová, Renata - Kuglík, Petr
PY  - 2021
TI  - Case Report: Contiguous Xq22.3 Deletion Associated with ATS-ID Syndrome: From Genotype to Further Delineation of the Phenotype
JF  - Frontiers in Genetics
VL  - 12
IS  - October
SP  - 750110
EP  - 750110
PB  - Frontiers Media S.A.
SN  - 16648021
KW  - ATS-MR syndrome
KW  - trio-based whole exome sequencing
KW  - genotype-phenotype analysis
KW  - neurodevelopmental disorders
KW  - Xq22.3q23 deletions
UR  - https://doi.org/10.3389/fgene.2021.750110
N2  - Alport syndrome with intellectual disability (ATS-ID, AMME complex; OMIM #300194) is an X-linked contiguous gene deletion syndrome associated with an Xq22.3 locus mainly characterized by hematuria, renal failure, hearing loss/deafness, neurodevelopmental disorder (NDD), midface retrusion, and elliptocytosis. It is thought that ATS-ID is caused by the loss of function of COL4A5 (ATS) and FACL4 (ACSL4) genes through the interstitial (micro)deletion of chromosomal band Xq22.3. We report detailed phenotypic description and results from genome-wide screening of a Czech family with diagnosis ATS-ID (proband, maternal uncle, and two female carriers). Female carriers showed mild clinical features of microscopic hematuria only, while affected males displayed several novel clinical features associated with ATS-ID. Utilization of whole-exome sequencing discovered the presence of approximately 3 Mb of deletion in the Xq23 area, which affected 19 genes from TSC22D3 to CHRDL1. We compared the clinical phenotype with previously reported three ATS-ID families worldwide and correlated their clinical manifestations with the incidence of genes in both telomeric and centromeric regions of the deleted chromosomal area. In addition to previously described phenotypes associated with aberrations in AMMECR1 and FACL4, we identified two genes, members of tripartite motif family MID2 and subunit of the proteasome PA700/19S complex (PSMD10), respectively, as prime candidate genes responsible for additional clinical features observed in our patients with ATS-ID. Overall, our findings further improve the knowledge about the clinical impact of Xq23 deletions and bring novel information about phenotype/genotype association of this chromosomal aberration.
ER  -

SMETANA, Jan; Vladimíra VALLOVÁ; Markéta WAYHELOVÁ; Eva HLADÍLKOVÁ; Hana FILKOVÁ; Věra HOŘÍNOVÁ; Petr BROŽ; Aneta MIKULÁŠOVÁ; Renata GAILLYOVÁ a Petr KUGLÍK. Case Report: Contiguous Xq22.3 Deletion Associated with ATS-ID Syndrome: From Genotype to Further Delineation of the Phenotype. \textit{Frontiers in Genetics}. Frontiers Media S.A., 2021, roč.~12, October, s.~750110-750116. ISSN~1664-8021. Dostupné z: https://doi.org/10.3389/fgene.2021.750110.

Přehled o publikaci