Expanding the genetic heterogeneity of intellectual disability

被引：117

作者：

Anazi, Shams ^{[1
]}

Maddirevula, Sateesh ^{[1
]}

Salpietro, Vincenzo ^{[23
]}

Asi, Yasmine T. ^{[2
]}

Alsahli, Saud ^{[1
]}

Alhashem, Amal ^{[3
]}

Shamseldin, Hanan E. ^{[1
]}

AlZahrani, Fatema ^{[1
]}

Patel, Nisha ^{[1
]}

Ibrahim, Niema ^{[1
]}

Abdulwahab, Firdous M. ^{[1
]}

Hashem, Mais ^{[1
]}

Alhashmi, Nadia ^{[4
]}

Al Murshedi, Fathiya ^{[4
]}

Al Kindy, Adila ^{[4
]}

Alshaer, Ahmad ^{[13
]}

Rumayyan, Ahmed ^{[5
,6
]}

Al Tala, Saeed ^{[7
,8
]}

Kurdi, Wesam ^{[9
]}

Alsaman, Abdulaziz ^{[18
]}

Alasmari, Ali ^{[18
]}

Banu, Selina ^{[24
]}

Sultan, Tipu ^{[25
,26
]}

Saleh, Mohammed M. ^{[18
]}

Alkuraya, Hisham ^{[10
]}

Salih, Mustafa A. ^{[11
,12
]}

Aldhalaan, Hesham ^{[13
]}

Ben-Omran, Tawfeg ^{[14
]}

Al Musafri, Fatima ^{[14
]}

Ali, Rehab ^{[14
]}

Suleiman, Jehan ^{[15
]}

Tabarki, Brahim ^{[3
]}

El-Hattab, Ayman W. ^{[16
]}

Bupp, Caleb ^{[19
]}

Alfadhel, Majid ^{[20
]}

Al Tassan, Nada ^{[1
,17
]}

Monies, Dorota ^{[1
,17
]}

Arold, Stefan T. ^{[21
,22
]}

Abouelhoda, Mohamed ^{[1
,17
]}

Lashley, Tammaryn ^{[2
]}

Houlden, Henry ^{[23
]}

Faqeih, Eissa ^{[18
]}

Alkuraya, Fowzan S. ^{[1
,3
,17
,19
,22
]}

机构：

[1] King Faisal Specialist Hosp & Res Ctr, Dept Genet, Riyadh, Saudi Arabia

[2] UCL, UCL Inst Neurol, Queen Sq Brain Bank Neurol Disorders, Dept Mol Neurosci, London, England

[3] Prince Sultan Mil Med City, Dept Pediat, Riyadh, Saudi Arabia

[4] Sultan Qaboos Univ, Coll Med, Dept Genet, Muscat, Oman

[5] King Saud bin Abdulaziz Univ Hlth Sci, Riyadh, Saudi Arabia

[6] King Abdul Aziz Med City, Dept Pediat, Neurol Div, Riyadh, Saudi Arabia

[7] Armed Forces Hosp, Dept Pediat, Khamis Mushayt, Saudi Arabia

[8] Armed Forces Hosp, Genet Unit, Khamis Mushayt, Saudi Arabia

[9] King Faisal Specialist Hosp & Res Ctr, Dept Obstet & Gynecol, Riyadh, Saudi Arabia

[10] Specialized Med Ctr Hosp, Dept Ophthalmol, Riyadh, Saudi Arabia

[11] King Saud Univ, King Khalid Univ Hosp, Dept Pediat, Div Pediat Neurol, Riyadh, Saudi Arabia

[12] King Saud Univ, Coll Med, Riyadh, Saudi Arabia

[13] King Faisal Specialist Hosp & Res Ctr, Pediat Neurol, Riyadh, Saudi Arabia

[14] Hamad Med Corp, Dept Pediat, Clin & Metab Genet, Doha, Qatar

[15] Tawam Hosp, Div Neurol, Dept Pediat, Al Ain, U Arab Emirates

[16] Tawam Hosp, Dept Pediat, Div Clin Genet & Metab Disorders, Al Ain, U Arab Emirates

[17] King Abdulaziz City Sci & Technol, Saudi Human Genome Program, Riyadh, Saudi Arabia

[18] King Fahad Med City, Childrens Hosp, Dept Pediat Subspecialties, Riyadh, Saudi Arabia

[19] Spectrum Hlth Genet, Grand Rapids, MI 49503 USA

[20] King Saud bin Abdulaziz Univ Hlth Sci, King Abdullah Int Med Res Ctr, Dept Pediat, Genet Div,King Abdulaziz Med City, Riyadh, Saudi Arabia

[21] King Abdullah Univ Sci & Technol, Computat Biosci Res Ctr, Div Biol & Environm Sci & Engn BESE, Thuwal 239556900, Saudi Arabia

[22] King Abdullah Univ Sci & Technol, Div Biol & Environm Sci & Engn BESE, Thuwal 239556900, Saudi Arabia

[23] UCL Inst Neurol, Dept Mol Neurosci, London, England

[24] ICH & SSF Hosp Mirpur, Dept Pediat, Dhaka 1216, Bangladesh

[25] Inst Child Hlth, Dept Pediat Neurol, 381-D-2, Lahore, Pakistan

[26] Childrens Hosp Lahore, 381-D-2, Lahore, Pakistan

来源：

HUMAN GENETICS | 2017年 / 136卷 / 11-12期

关键词：

PROTEIN; MUTATION; DISEASE; NKCC1; VARIANTS; EXCHANGE; INSIGHTS; SLC12A2; BRAIN;

D O I：

10.1007/s00439-017-1843-2

中图分类号：

Q3 [遗传学];

学科分类号：

071007 ; 090102 ;

摘要：

Intellectual disability (ID) is a common morbid condition with a wide range of etiologies. The list of monogenic forms of ID has increased rapidly in recent years thanks to the implementation of genomic sequencing techniques. In this study, we describe the phenotypic and genetic findings of 68 families (105 patients) all with novel IDrelated variants. In addition to established ID genes, including ones for which we describe unusual mutational mechanism, some of these variants represent the first confirmatory disease-gene links following previous reports (TRAK1, GTF3C3, SPTBN4 and NKX6-2), some of which were based on single families. Furthermore, we describe novel variants in 14 genes that we propose as novel candidates (ANKHD1, ASTN2, ATP13A1, FMO4, MADD, MFSD11, NCKAP1, NFASC, PCDHGA10, PPP1R21, SLC12A2, SLK, STK32C and ZFAT). We highlight MADD and PCDHGA10 as particularly compelling candidates in which we identified biallelic likely deleterious variants in two independent ID families each. We also highlight NCKAP1 as another compelling candidate in a large family with autosomal dominant mild intellectual disability that fully segregates with a heterozygous truncating variant. The candidacy of NCKAP1 is further supported by its biological function, and our demonstration of relevant expression in human brain. Our study expands the locus and allelic heterogeneity of ID and demonstrates the power of positional mapping to reveal unusual mutational mechanisms.

引用

页码：1419 / 1429

页数：11

共 44 条

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