TY - JOUR
T1 - Further delineation of BCAP31-linked intellectual disability
T2 - description of 17 new families with LoF and missense variants
AU - Care4Rare Canada Consortium
AU - Whalen, Sandra
AU - Shaw, Marie
AU - Mignot, Cyril
AU - Héron, Delphine
AU - Bastaraud, Sandra Chantot
AU - Walti, Cecile Cieuta
AU - Liebelt, Jan
AU - Elmslie, Frances
AU - Yap, Patrick
AU - Hurst, Jane
AU - Forsythe, Elisabeth
AU - Kirmse, Brian
AU - Ozmore, Jillian
AU - Spinelli, Alessandro Mauro
AU - Calabrese, Olga
AU - de Villemeur, Thierry Billette
AU - Tabet, Anne Claude
AU - Levy, Jonathan
AU - Guet, Agnes
AU - Kossorotoff, Manoëlle
AU - Kamien, Benjamin
AU - Morton, Jenny
AU - McCabe, Anne
AU - Brischoux-Boucher, Elise
AU - Raas-Rothschild, Annick
AU - Pini, Antonella
AU - Carroll, Renée
AU - Hartley, Jessica N.
AU - Boycott, Kym
AU - Brudno, Michael
AU - Bernier, Francois
AU - van Karnebeek, Clara
AU - Dyment, David
AU - Kernohan, Kristin
AU - Innes, Micheil
AU - Lamont, Ryan
AU - Parboosingh, Jillian
AU - Marshall, Deborah
AU - Marshall, Christian
AU - Mendoza, Roberto
AU - Dowling, James
AU - Hayeems, Robin
AU - Knoppers, Bartha
AU - Lehman, Anna
AU - Mostafavi, Sara
AU - Frosk, Patrick
AU - Slavotinek, Anne
AU - Truxal, Kristen
AU - Jennifer, Carroll
AU - Dheedene, Annelies
N1 - Publisher Copyright:
© 2021, The Author(s), under exclusive licence to European Society of Human Genetics.
PY - 2021/9
Y1 - 2021/9
N2 - The BCAP31 gene, located at Xq28, encodes BAP31, which plays a role in ER-to-Golgi anterograde transport. To date, BCAP31 pathogenic variants have been reported in 12 male cases from seven families (six loss of function (LoF) and one missense). Patients had severe intellectual disability (ID), dystonia, deafness, and central hypomyelination, delineating a so-called deafness, dystonia and cerebral hypomyelination syndrome (DDCH). Female carriers are mostly asymptomatic but may present with deafness. BCAP31 is flanked by the SLC6A8 and ABCD1 genes. Contiguous deletions of BCAP31 and ABCD1 and/or SLC6A8 have been described in 12 patients. Patients with deletions including BCAP31 and SLC6A8 have the same phenotype as BCAP31 patients. Patients with deletions of BCAP31 and ABCD1 have contiguous ABCD1 and DXS1375E/BCAP31 deletion syndrome (CADDS), and demonstrate a more severe neurological phenotype with cholestatic liver disease and early death. We report 17 novel families, 14 with intragenic BCAP31 variants (LoF and missense) and three with a deletion of BCAP31 and adjacent genes (comprising two CADDS patients, one male and one symptomatic female). Our study confirms the phenotype reported in males with intragenic LoF variants and shows that males with missense variants exhibit a milder phenotype. Most patients with a LoF pathogenic BCAP31 variant have permanent or transient liver enzyme elevation. We further demonstrate that carrier females (n = 10) may have a phenotype comprising LD, ID, and/or deafness. The male with CADDS had a severe neurological phenotype, but no cholestatic liver disease, and the symptomatic female had moderate ID and cholestatic liver disease.
AB - The BCAP31 gene, located at Xq28, encodes BAP31, which plays a role in ER-to-Golgi anterograde transport. To date, BCAP31 pathogenic variants have been reported in 12 male cases from seven families (six loss of function (LoF) and one missense). Patients had severe intellectual disability (ID), dystonia, deafness, and central hypomyelination, delineating a so-called deafness, dystonia and cerebral hypomyelination syndrome (DDCH). Female carriers are mostly asymptomatic but may present with deafness. BCAP31 is flanked by the SLC6A8 and ABCD1 genes. Contiguous deletions of BCAP31 and ABCD1 and/or SLC6A8 have been described in 12 patients. Patients with deletions including BCAP31 and SLC6A8 have the same phenotype as BCAP31 patients. Patients with deletions of BCAP31 and ABCD1 have contiguous ABCD1 and DXS1375E/BCAP31 deletion syndrome (CADDS), and demonstrate a more severe neurological phenotype with cholestatic liver disease and early death. We report 17 novel families, 14 with intragenic BCAP31 variants (LoF and missense) and three with a deletion of BCAP31 and adjacent genes (comprising two CADDS patients, one male and one symptomatic female). Our study confirms the phenotype reported in males with intragenic LoF variants and shows that males with missense variants exhibit a milder phenotype. Most patients with a LoF pathogenic BCAP31 variant have permanent or transient liver enzyme elevation. We further demonstrate that carrier females (n = 10) may have a phenotype comprising LD, ID, and/or deafness. The male with CADDS had a severe neurological phenotype, but no cholestatic liver disease, and the symptomatic female had moderate ID and cholestatic liver disease.
UR - http://www.scopus.com/inward/record.url?scp=85101167280&partnerID=8YFLogxK
U2 - 10.1038/s41431-021-00821-0
DO - 10.1038/s41431-021-00821-0
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C2 - 33603160
AN - SCOPUS:85101167280
SN - 1018-4813
VL - 29
SP - 1405
EP - 1417
JO - European Journal of Human Genetics
JF - European Journal of Human Genetics
IS - 9
ER -