A mutation affecting laminin alpha 5 polymerisation gives rise to a syndromic developmental disorder

Lynelle K. Jones; Rachel Lam; Karen K. McKee; Maya Aleksandrova; John Dowling; Stephen I. Alexander; Amali Mallawaarachchi; Denny L. Cottle; Kieran M. Short; Lynn Pais; Jeffery H. Miner; Andrew J. Mallett; Cas Simons; Hugh McCarthy; Peter D. Yurchenco; Ian M. Smyth

doi:10.1242/dev.189183

A mutation affecting laminin alpha 5 polymerisation gives rise to a syndromic developmental disorder

Lynelle K. Jones, Rachel Lam, Karen K. McKee, Maya Aleksandrova, John Dowling, Stephen I. Alexander, Amali Mallawaarachchi, Denny L. Cottle, Kieran M. Short, Lynn Pais, Jeffery H. Miner, Andrew J. Mallett, Cas Simons, Hugh McCarthy, Peter D. Yurchenco, Ian M. Smyth

Research output: Contribution to journal › Article › peer-review

18 Scopus citations

Abstract

Laminin alpha 5 (LAMA5) is a member of a large family of proteins that trimerise and then polymerise to form a central component of all basement membranes. Consequently, the protein plays an instrumental role in shaping the normal development of the kidney, skin, neural tube, lung and limb, and many other organs and tissues. Pathogenic mutations in some laminins have been shown to cause a range of largely syndromic conditions affecting the competency of the basement membranes to which they contribute. We report the identification of a mutation in the polymerisation domain of LAMA5 in a patient with a complex syndromic disease characterised by defects in kidney, craniofacial and limb development, and by a range of other congenital defects. Using CRISPR-generated mouse models and biochemical assays, we demonstrate the pathogenicity of this variant, showing that the change results in a failure of the polymerisation of α/β/γ laminin trimers. Comparing these in vivo phenotypes with those apparent upon gene deletion in mice provides insights into the specific functional importance of laminin polymerisation during development and tissue homeostasis.

Original language	English
Article number	dev189183
Journal	Development (Cambridge)
Volume	147
Issue number	21
DOIs	https://doi.org/10.1242/dev.189183
State	Published - Nov 2020

Keywords

Basement membrane
Kidney
LAMA5
Laminin alpha 5
Laminin polymerisation

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10.1242/dev.189183

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Jones, L. K., Lam, R., McKee, K. K., Aleksandrova, M., Dowling, J., Alexander, S. I., Mallawaarachchi, A., Cottle, D. L., Short, K. M., Pais, L., Miner, J. H., Mallett, A. J., Simons, C., McCarthy, H., Yurchenco, P. D., & Smyth, I. M. (2020). A mutation affecting laminin alpha 5 polymerisation gives rise to a syndromic developmental disorder. Development (Cambridge), 147(21), Article dev189183. https://doi.org/10.1242/dev.189183

@article{f8a3e647cc254ece8327fd8060044759,

title = "A mutation affecting laminin alpha 5 polymerisation gives rise to a syndromic developmental disorder",

abstract = "Laminin alpha 5 (LAMA5) is a member of a large family of proteins that trimerise and then polymerise to form a central component of all basement membranes. Consequently, the protein plays an instrumental role in shaping the normal development of the kidney, skin, neural tube, lung and limb, and many other organs and tissues. Pathogenic mutations in some laminins have been shown to cause a range of largely syndromic conditions affecting the competency of the basement membranes to which they contribute. We report the identification of a mutation in the polymerisation domain of LAMA5 in a patient with a complex syndromic disease characterised by defects in kidney, craniofacial and limb development, and by a range of other congenital defects. Using CRISPR-generated mouse models and biochemical assays, we demonstrate the pathogenicity of this variant, showing that the change results in a failure of the polymerisation of α/β/γ laminin trimers. Comparing these in vivo phenotypes with those apparent upon gene deletion in mice provides insights into the specific functional importance of laminin polymerisation during development and tissue homeostasis.",

keywords = "Basement membrane, Kidney, LAMA5, Laminin alpha 5, Laminin polymerisation",

author = "Jones, {Lynelle K.} and Rachel Lam and McKee, {Karen K.} and Maya Aleksandrova and John Dowling and Alexander, {Stephen I.} and Amali Mallawaarachchi and Cottle, {Denny L.} and Short, {Kieran M.} and Lynn Pais and Miner, {Jeffery H.} and Mallett, {Andrew J.} and Cas Simons and Hugh McCarthy and Yurchenco, {Peter D.} and Smyth, {Ian M.}",

note = "Funding Information: A.J.M. has received research grant funding from Sanofi-Genzyme and has membership of an Advisory Board for Otsuka, neither of which are related to this project or work. Funding Information: The studies were performed using the expertise, equipment and reagents of several Monash University Research Platforms including the Monash Genome Modification Platform (incorporating the Australian Phenomics Network), Monash Animal Research Platform, Monash Microimaging, the Ramaciotti Centre for Cryo-Electron Microscopy and the Monash Histology Platform. We are indebted to the patients and families involved and to the clinical, diagnostic and research staff of the KidGen Collaborative. The KidGen Collaborative Flagship is supported by the Melbourne Genomics Health Alliance (Melbourne Genomics), grants from the Royal Children{\textquoteright}s Hospital Foundation and Royal Brisbane and Women{\textquoteright}s Hospital Foundation and by the National Health and Medical Research Council Genomics TCR Grant 1113531, entitled {\textquoteleft}Preparing Australia for Genomic Medicine: A proposal by the Australian Genomics Health Alliance{\textquoteright}. Melbourne Genomics is funded by the 10 members and the State Government of Victoria (Department of Health and Humans Services). In-kind funding support was provided for renal genetics clinic operation and genomic test provision by Queensland Health (Metro North Hospital and Health Service; Children{\textquoteright}s Health Queensland Hospital and Health Service), New South Wales Health, South Australia Health, Western Australia Department of Health, Northern Territory Department of Health and Tasmanian Department of Health and Human Services. The production of mouse lines in this study were subsidised by the Australian Phenomics Network which is supported by the Australian Government through the National Collaborative Research Infrastructure Strategy (NCRIS) Program. Funding for sequencing was provided by CostCo to the Sydney Children{\textquoteright}s Hospital Network and the Centre for Kidney Research. The research conducted at the Murdoch Children{\textquoteright}s Research Institute was supported by the Victorian Government{\textquoteright}s Operational Infrastructure Support Program. Sequencing and analysis were provided by the Broad Institute of MIT and Harvard Center for Mendelian Genomics (Broad CMG) and was funded by the National Human Genome Research Institute, the National Eye Institute, and the National Heart, Lung and Blood Institute (UM1 HG008900) and in part by the National Human Genome Research Institute grant R01 HG009141. Publisher Copyright: {\textcopyright} 2020. Published by The Company of Biologists Ltd",

year = "2020",

month = nov,

doi = "10.1242/dev.189183",

language = "English",

volume = "147",

journal = "Development (Cambridge)",

issn = "0950-1991",

number = "21",

}

Jones, LK, Lam, R, McKee, KK, Aleksandrova, M, Dowling, J, Alexander, SI, Mallawaarachchi, A, Cottle, DL, Short, KM, Pais, L, Miner, JH, Mallett, AJ, Simons, C, McCarthy, H, Yurchenco, PD & Smyth, IM 2020, 'A mutation affecting laminin alpha 5 polymerisation gives rise to a syndromic developmental disorder', Development (Cambridge), vol. 147, no. 21, dev189183. https://doi.org/10.1242/dev.189183

TY - JOUR

T1 - A mutation affecting laminin alpha 5 polymerisation gives rise to a syndromic developmental disorder

AU - Jones, Lynelle K.

AU - Lam, Rachel

AU - McKee, Karen K.

AU - Aleksandrova, Maya

AU - Dowling, John

AU - Alexander, Stephen I.

AU - Mallawaarachchi, Amali

AU - Cottle, Denny L.

AU - Short, Kieran M.

AU - Pais, Lynn

AU - Miner, Jeffery H.

AU - Mallett, Andrew J.

AU - Simons, Cas

AU - McCarthy, Hugh

AU - Yurchenco, Peter D.

AU - Smyth, Ian M.

N1 - Funding Information: A.J.M. has received research grant funding from Sanofi-Genzyme and has membership of an Advisory Board for Otsuka, neither of which are related to this project or work. Funding Information: The studies were performed using the expertise, equipment and reagents of several Monash University Research Platforms including the Monash Genome Modification Platform (incorporating the Australian Phenomics Network), Monash Animal Research Platform, Monash Microimaging, the Ramaciotti Centre for Cryo-Electron Microscopy and the Monash Histology Platform. We are indebted to the patients and families involved and to the clinical, diagnostic and research staff of the KidGen Collaborative. The KidGen Collaborative Flagship is supported by the Melbourne Genomics Health Alliance (Melbourne Genomics), grants from the Royal Children’s Hospital Foundation and Royal Brisbane and Women’s Hospital Foundation and by the National Health and Medical Research Council Genomics TCR Grant 1113531, entitled ‘Preparing Australia for Genomic Medicine: A proposal by the Australian Genomics Health Alliance’. Melbourne Genomics is funded by the 10 members and the State Government of Victoria (Department of Health and Humans Services). In-kind funding support was provided for renal genetics clinic operation and genomic test provision by Queensland Health (Metro North Hospital and Health Service; Children’s Health Queensland Hospital and Health Service), New South Wales Health, South Australia Health, Western Australia Department of Health, Northern Territory Department of Health and Tasmanian Department of Health and Human Services. The production of mouse lines in this study were subsidised by the Australian Phenomics Network which is supported by the Australian Government through the National Collaborative Research Infrastructure Strategy (NCRIS) Program. Funding for sequencing was provided by CostCo to the Sydney Children’s Hospital Network and the Centre for Kidney Research. The research conducted at the Murdoch Children’s Research Institute was supported by the Victorian Government’s Operational Infrastructure Support Program. Sequencing and analysis were provided by the Broad Institute of MIT and Harvard Center for Mendelian Genomics (Broad CMG) and was funded by the National Human Genome Research Institute, the National Eye Institute, and the National Heart, Lung and Blood Institute (UM1 HG008900) and in part by the National Human Genome Research Institute grant R01 HG009141. Publisher Copyright: © 2020. Published by The Company of Biologists Ltd

PY - 2020/11

Y1 - 2020/11

N2 - Laminin alpha 5 (LAMA5) is a member of a large family of proteins that trimerise and then polymerise to form a central component of all basement membranes. Consequently, the protein plays an instrumental role in shaping the normal development of the kidney, skin, neural tube, lung and limb, and many other organs and tissues. Pathogenic mutations in some laminins have been shown to cause a range of largely syndromic conditions affecting the competency of the basement membranes to which they contribute. We report the identification of a mutation in the polymerisation domain of LAMA5 in a patient with a complex syndromic disease characterised by defects in kidney, craniofacial and limb development, and by a range of other congenital defects. Using CRISPR-generated mouse models and biochemical assays, we demonstrate the pathogenicity of this variant, showing that the change results in a failure of the polymerisation of α/β/γ laminin trimers. Comparing these in vivo phenotypes with those apparent upon gene deletion in mice provides insights into the specific functional importance of laminin polymerisation during development and tissue homeostasis.

AB - Laminin alpha 5 (LAMA5) is a member of a large family of proteins that trimerise and then polymerise to form a central component of all basement membranes. Consequently, the protein plays an instrumental role in shaping the normal development of the kidney, skin, neural tube, lung and limb, and many other organs and tissues. Pathogenic mutations in some laminins have been shown to cause a range of largely syndromic conditions affecting the competency of the basement membranes to which they contribute. We report the identification of a mutation in the polymerisation domain of LAMA5 in a patient with a complex syndromic disease characterised by defects in kidney, craniofacial and limb development, and by a range of other congenital defects. Using CRISPR-generated mouse models and biochemical assays, we demonstrate the pathogenicity of this variant, showing that the change results in a failure of the polymerisation of α/β/γ laminin trimers. Comparing these in vivo phenotypes with those apparent upon gene deletion in mice provides insights into the specific functional importance of laminin polymerisation during development and tissue homeostasis.

KW - Basement membrane

KW - Kidney

KW - LAMA5

KW - Laminin alpha 5

KW - Laminin polymerisation

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U2 - 10.1242/dev.189183

DO - 10.1242/dev.189183

M3 - Article

C2 - 32439764

AN - SCOPUS:85097319207

SN - 0950-1991

VL - 147

JO - Development (Cambridge)

JF - Development (Cambridge)

IS - 21

M1 - dev189183

ER -

A mutation affecting laminin alpha 5 polymerisation gives rise to a syndromic developmental disorder

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Keywords

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