A case series of familial ARID1B variants illustrating variable expression and suggestions to update the ACMG criteria

Pleuntje J. van der Sluijs; Mariëlle Alders; Alexander J. M. Dingemans; Kareesma Parbhoo; Bregje W. van Bon; Jennifer C. Dempsey; Dan Doherty; Johan T. den Dunnen; Erica H. Gerkes; Ilana M. Milller; Stephanie Moortgat; Debra S. Regier; Claudia A. L. Ruivenkamp; Betsy Schmalz; Thomas Smol; Kyra E. Stuurman; Catherine Vincent-Delorme; Bert B. A. de Vries; Bekim Sadikovic; Scott E. Hickey; Jill A. Rosenfeld; Isabelle Maystadt; Gijs W. E. Santen

doi:https://doi.org/10.3390/genes12081275

A case series of familial ARID1B variants illustrating variable expression and suggestions to update the ACMG criteria

Pleuntje J. van der Sluijs, Mariëlle Alders, Alexander J. M. Dingemans, Kareesma Parbhoo, Bregje W. van Bon, Jennifer C. Dempsey, Dan Doherty, Johan T. den Dunnen, Erica H. Gerkes, Ilana M. Milller, Stephanie Moortgat, Debra S. Regier, Claudia A. L. Ruivenkamp, Betsy Schmalz, Thomas Smol, Kyra E. Stuurman, Catherine Vincent-Delorme, Bert B. A. de Vries, Bekim Sadikovic, Scott E. HickeyJill A. Rosenfeld, Isabelle Maystadt, Gijs W. E. Santen

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Abstract

ARID1B is one of the most frequently mutated genes in intellectual disability (~1%). Most variants are readily classified, since they are de novo and are predicted to lead to loss of function, and therefore classified as pathogenic according to the American College of Medical Genetics and Genomics (ACMG) guidelines for the interpretation of sequence variants. However, familial loss-of-function variants can also occur and can be challenging to interpret. Such variants may be pathogenic with variable expression, causing only a mild phenotype in a parent. Alternatively, since some regions of the ARID1B gene seem to be lacking pathogenic variants, loss-of-function variants in those regions may not lead to ARID1B haploinsufficiency and may therefore be benign. We describe 12 families with potential loss-of-function variants, which were either familial or with unknown inheritance and were in regions where pathogenic variants have not been described or are otherwise challenging to interpret. We performed detailed clinical and DNA methylation studies, which allowed us to confidently classify most variants. In five families we observed transmission of pathogenic variants, confirming their highly variable expression. Our findings provide further evidence for an alternative translational start site and we suggest updates for the ACMG guidelines for the interpretation of sequence variants to incorporate DNA methylation studies and facial analyses.

Original language	English
Article number	1275
Journal	Genes
Volume	12
Issue number	8
DOIs	https://doi.org/10.3390/genes12081275
Publication status	Published - 1 Aug 2021

Keywords

ACMG guidelines
ARID1B
Coffin–Siris syndrome
Familial
Inherited
Intellectual disability
Non-pathogenic
Variable expression

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van der Sluijs, P. J., Alders, M., Dingemans, A. J. M., Parbhoo, K., van Bon, B. W., Dempsey, J. C., Doherty, D., den Dunnen, J. T., Gerkes, E. H., Milller, I. M., Moortgat, S., Regier, D. S., Ruivenkamp, C. A. L., Schmalz, B., Smol, T., Stuurman, K. E., Vincent-Delorme, C., de Vries, B. B. A., Sadikovic, B., ... Santen, G. W. E. (2021). A case series of familial ARID1B variants illustrating variable expression and suggestions to update the ACMG criteria. Genes, 12(8), Article 1275. https://doi.org/10.3390/genes12081275

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title = "A case series of familial ARID1B variants illustrating variable expression and suggestions to update the ACMG criteria",

abstract = "ARID1B is one of the most frequently mutated genes in intellectual disability (~1%). Most variants are readily classified, since they are de novo and are predicted to lead to loss of function, and therefore classified as pathogenic according to the American College of Medical Genetics and Genomics (ACMG) guidelines for the interpretation of sequence variants. However, familial loss-of-function variants can also occur and can be challenging to interpret. Such variants may be pathogenic with variable expression, causing only a mild phenotype in a parent. Alternatively, since some regions of the ARID1B gene seem to be lacking pathogenic variants, loss-of-function variants in those regions may not lead to ARID1B haploinsufficiency and may therefore be benign. We describe 12 families with potential loss-of-function variants, which were either familial or with unknown inheritance and were in regions where pathogenic variants have not been described or are otherwise challenging to interpret. We performed detailed clinical and DNA methylation studies, which allowed us to confidently classify most variants. In five families we observed transmission of pathogenic variants, confirming their highly variable expression. Our findings provide further evidence for an alternative translational start site and we suggest updates for the ACMG guidelines for the interpretation of sequence variants to incorporate DNA methylation studies and facial analyses.",

keywords = "ACMG guidelines, ARID1B, Coffin–Siris syndrome, Familial, Inherited, Intellectual disability, Non-pathogenic, Variable expression",

author = "{van der Sluijs}, {Pleuntje J.} and Mari{\"e}lle Alders and Dingemans, {Alexander J. M.} and Kareesma Parbhoo and {van Bon}, {Bregje W.} and Dempsey, {Jennifer C.} and Dan Doherty and {den Dunnen}, {Johan T.} and Gerkes, {Erica H.} and Milller, {Ilana M.} and Stephanie Moortgat and Regier, {Debra S.} and Ruivenkamp, {Claudia A. L.} and Betsy Schmalz and Thomas Smol and Stuurman, {Kyra E.} and Catherine Vincent-Delorme and {de Vries}, {Bert B. A.} and Bekim Sadikovic and Hickey, {Scott E.} and Rosenfeld, {Jill A.} and Isabelle Maystadt and Santen, {Gijs W. E.}",

note = "Publisher Copyright: {\textcopyright} 2021 by the authors. Licensee MDPI, Basel, Switzerland.",

year = "2021",

month = aug,

day = "1",

doi = "https://doi.org/10.3390/genes12081275",

language = "English",

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van der Sluijs, PJ, Alders, M, Dingemans, AJM, Parbhoo, K, van Bon, BW, Dempsey, JC, Doherty, D, den Dunnen, JT, Gerkes, EH, Milller, IM, Moortgat, S, Regier, DS, Ruivenkamp, CAL, Schmalz, B, Smol, T, Stuurman, KE, Vincent-Delorme, C, de Vries, BBA, Sadikovic, B, Hickey, SE, Rosenfeld, JA, Maystadt, I & Santen, GWE 2021, 'A case series of familial ARID1B variants illustrating variable expression and suggestions to update the ACMG criteria', Genes, vol. 12, no. 8, 1275. https://doi.org/10.3390/genes12081275

TY - JOUR

T1 - A case series of familial ARID1B variants illustrating variable expression and suggestions to update the ACMG criteria

AU - van der Sluijs, Pleuntje J.

AU - Alders, Mariëlle

AU - Dingemans, Alexander J. M.

AU - Parbhoo, Kareesma

AU - van Bon, Bregje W.

AU - Dempsey, Jennifer C.

AU - Doherty, Dan

AU - den Dunnen, Johan T.

AU - Gerkes, Erica H.

AU - Milller, Ilana M.

AU - Moortgat, Stephanie

AU - Regier, Debra S.

AU - Ruivenkamp, Claudia A. L.

AU - Schmalz, Betsy

AU - Smol, Thomas

AU - Stuurman, Kyra E.

AU - Vincent-Delorme, Catherine

AU - de Vries, Bert B. A.

AU - Sadikovic, Bekim

AU - Hickey, Scott E.

AU - Rosenfeld, Jill A.

AU - Maystadt, Isabelle

AU - Santen, Gijs W. E.

PY - 2021/8/1

Y1 - 2021/8/1

N2 - ARID1B is one of the most frequently mutated genes in intellectual disability (~1%). Most variants are readily classified, since they are de novo and are predicted to lead to loss of function, and therefore classified as pathogenic according to the American College of Medical Genetics and Genomics (ACMG) guidelines for the interpretation of sequence variants. However, familial loss-of-function variants can also occur and can be challenging to interpret. Such variants may be pathogenic with variable expression, causing only a mild phenotype in a parent. Alternatively, since some regions of the ARID1B gene seem to be lacking pathogenic variants, loss-of-function variants in those regions may not lead to ARID1B haploinsufficiency and may therefore be benign. We describe 12 families with potential loss-of-function variants, which were either familial or with unknown inheritance and were in regions where pathogenic variants have not been described or are otherwise challenging to interpret. We performed detailed clinical and DNA methylation studies, which allowed us to confidently classify most variants. In five families we observed transmission of pathogenic variants, confirming their highly variable expression. Our findings provide further evidence for an alternative translational start site and we suggest updates for the ACMG guidelines for the interpretation of sequence variants to incorporate DNA methylation studies and facial analyses.

AB - ARID1B is one of the most frequently mutated genes in intellectual disability (~1%). Most variants are readily classified, since they are de novo and are predicted to lead to loss of function, and therefore classified as pathogenic according to the American College of Medical Genetics and Genomics (ACMG) guidelines for the interpretation of sequence variants. However, familial loss-of-function variants can also occur and can be challenging to interpret. Such variants may be pathogenic with variable expression, causing only a mild phenotype in a parent. Alternatively, since some regions of the ARID1B gene seem to be lacking pathogenic variants, loss-of-function variants in those regions may not lead to ARID1B haploinsufficiency and may therefore be benign. We describe 12 families with potential loss-of-function variants, which were either familial or with unknown inheritance and were in regions where pathogenic variants have not been described or are otherwise challenging to interpret. We performed detailed clinical and DNA methylation studies, which allowed us to confidently classify most variants. In five families we observed transmission of pathogenic variants, confirming their highly variable expression. Our findings provide further evidence for an alternative translational start site and we suggest updates for the ACMG guidelines for the interpretation of sequence variants to incorporate DNA methylation studies and facial analyses.

KW - ACMG guidelines

KW - ARID1B

KW - Coffin–Siris syndrome

KW - Familial

KW - Inherited

KW - Intellectual disability

KW - Non-pathogenic

KW - Variable expression

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U2 - https://doi.org/10.3390/genes12081275

DO - https://doi.org/10.3390/genes12081275

M3 - Article

C2 - 34440449

SN - 2073-4425

VL - 12

JO - Genes

JF - Genes

IS - 8

M1 - 1275

ER -

A case series of familial ARID1B variants illustrating variable expression and suggestions to update the ACMG criteria

Abstract

Keywords

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