SemOpenAlex |

SemOpenAlex

Matches in SemOpenAlex for { <https://semopenalex.org/work/W1552016186> ?p ?o ?g. }

Showing items 1 to 100 of ±181 with 100 items per page.

W1552016186 endingPage "397" @default.
W1552016186 startingPage "385" @default.
W1552016186 abstract "The methyl-CpG-binding domain (MBD) gene family was first linked to autism over a decade ago when Rett syndrome, which falls under the umbrella of autism spectrum disorders (ASDs), was revealed to be predominantly caused by MECP2 mutations. Since that time, MECP2 alterations have been recognized in idiopathic ASD patients by us and others. Individuals with deletions across the MBD5 gene also present with ASDs, impaired speech, intellectual difficulties, repetitive behaviors, and epilepsy. These findings suggest that further investigations of the MBD gene family may reveal additional associations related to autism. We now describe the first study evaluating individuals with ASD for rare variants in four autosomal MBD family members, MBD5, MBD6, SETDB1, and SETDB2, and expand our initial screening in the MECP2 gene. Each gene was sequenced over all coding exons and evaluated for copy number variations in 287 patients with ASD and an equal number of ethnically matched control individuals. We identified 186 alterations through sequencing, approximately half of which were novel (96 variants, 51.6%). We identified 17 ASD specific, nonsynonymous variants, four of which were concordant in multiplex families: MBD5 Tyr1269Cys, MBD6 Arg883Trp, MECP2 Thr240Ser, and SETDB1 Pro1067del. Furthermore, a complex duplication spanning of the MECP2 gene was identified in two brothers who presented with developmental delay and intellectual disability. From our studies, we provide the first examples of autistic patients carrying potentially detrimental alterations in MBD6 and SETDB1, thereby demonstrating that the MBD gene family potentially plays a significant role in rare and private genetic causes of autism." @default.
W1552016186 created "2016-06-24" @default.
W1552016186 creator A5009558279 @default.
W1552016186 creator A5015846526 @default.
W1552016186 creator A5020266650 @default.
W1552016186 creator A5022844403 @default.
W1552016186 creator A5026352884 @default.
W1552016186 creator A5032798711 @default.
W1552016186 creator A5035696929 @default.
W1552016186 creator A5037844264 @default.
W1552016186 creator A5039221620 @default.
W1552016186 creator A5044153769 @default.
W1552016186 creator A5049398520 @default.
W1552016186 creator A5055324271 @default.
W1552016186 creator A5055461185 @default.
W1552016186 creator A5064752861 @default.
W1552016186 creator A5069324665 @default.
W1552016186 creator A5076736767 @default.
W1552016186 date "2012-10-10" @default.
W1552016186 modified "2023-10-16" @default.
W1552016186 title "The Expanding Role of MBD Genes in Autism: Identification of aMECP2Duplication and Novel Alterations inMBD5,MBD6, andSETDB1" @default.
W1552016186 cites W1511710204 @default.
W1552016186 cites W1559742681 @default.
W1552016186 cites W1964159332 @default.
W1552016186 cites W1965970535 @default.
W1552016186 cites W1967560377 @default.
W1552016186 cites W1968240088 @default.
W1552016186 cites W1970848271 @default.
W1552016186 cites W1976254276 @default.
W1552016186 cites W1980740976 @default.
W1552016186 cites W1980891541 @default.
W1552016186 cites W1985634754 @default.
W1552016186 cites W1988663056 @default.
W1552016186 cites W1993360322 @default.
W1552016186 cites W1993501734 @default.
W1552016186 cites W2000100376 @default.
W1552016186 cites W2002688255 @default.
W1552016186 cites W2005729136 @default.
W1552016186 cites W2010463957 @default.
W1552016186 cites W2013655994 @default.
W1552016186 cites W2013960233 @default.
W1552016186 cites W2015619933 @default.
W1552016186 cites W2020702702 @default.
W1552016186 cites W2024159278 @default.
W1552016186 cites W2031825131 @default.
W1552016186 cites W2032367255 @default.
W1552016186 cites W2033609439 @default.
W1552016186 cites W2035133243 @default.
W1552016186 cites W2038494883 @default.
W1552016186 cites W2039276157 @default.
W1552016186 cites W2042626978 @default.
W1552016186 cites W2044922756 @default.
W1552016186 cites W2046173010 @default.
W1552016186 cites W2059145105 @default.
W1552016186 cites W2061382200 @default.
W1552016186 cites W2063739474 @default.
W1552016186 cites W2065410176 @default.
W1552016186 cites W2067105766 @default.
W1552016186 cites W2071781936 @default.
W1552016186 cites W2072216690 @default.
W1552016186 cites W2073544062 @default.
W1552016186 cites W2074326406 @default.
W1552016186 cites W2079706646 @default.
W1552016186 cites W2084258753 @default.
W1552016186 cites W2092814182 @default.
W1552016186 cites W2101577241 @default.
W1552016186 cites W2106556368 @default.
W1552016186 cites W2106863904 @default.
W1552016186 cites W2107005658 @default.
W1552016186 cites W2108169091 @default.
W1552016186 cites W2112193800 @default.
W1552016186 cites W2112471545 @default.
W1552016186 cites W2115301408 @default.
W1552016186 cites W2120873167 @default.
W1552016186 cites W2125603023 @default.
W1552016186 cites W2127311839 @default.
W1552016186 cites W2127634492 @default.
W1552016186 cites W2128065392 @default.
W1552016186 cites W2130929529 @default.
W1552016186 cites W2134256373 @default.
W1552016186 cites W2137205471 @default.
W1552016186 cites W2140085473 @default.
W1552016186 cites W2145191876 @default.
W1552016186 cites W2146980885 @default.
W1552016186 cites W2149851863 @default.
W1552016186 cites W2150717926 @default.
W1552016186 cites W2155149522 @default.
W1552016186 cites W2155563035 @default.
W1552016186 cites W2155677754 @default.
W1552016186 cites W2157752701 @default.
W1552016186 cites W2161978970 @default.
W1552016186 cites W2222864307 @default.
W1552016186 cites W2937678484 @default.
W1552016186 doi "https://doi.org/10.1002/aur.1251" @default.
W1552016186 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/3528798" @default.
W1552016186 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/23055267" @default.
W1552016186 hasPublicationYear "2012" @default.
W1552016186 type Work @default.