Clinical characterization of patients with autosomal dominant short stature due to aggrecan mutations

Alexandra Gkourogianni; Melissa Andrew; Leah Tyzinski; Melissa Crocker; Jessica Douglas; Nancy Dunbar; Jan Fairchild; Mariana F.A. Funari; Karen E. Heath; Alexander A.L. Jorge; Tracey Kurtzman; Stephen LaFranchi; Seema Lalani; Jan Lebl; Yuezhen Lin; Evan Los; Dorothee Newbern; Catherine Nowak; Micah Olson; Jadranka Popovic; Stepanka Pruhova; Lenka Elblova; Jose Bernardo Quintos; Emma Segerlund; Lucia Sentchordi; Marwan Shinawi; Eva Lena Stattin; Jonathan Swartz; Ariadna Gonzalez Del Angel; Sinhue Diaz Cuellar; Hidekazu Hosono; Pedro A. Sanchez-Lara; Vivian Hwa; Jeffrey Baron; Ola Nilsson; Andrew Dauber

doi:10.1210/jc.2016-3313

Clinical characterization of patients with autosomal dominant short stature due to aggrecan mutations

Alexandra Gkourogianni, Melissa Andrew, Leah Tyzinski, Melissa Crocker, Jessica Douglas, Nancy Dunbar, Jan Fairchild, Mariana F.A. Funari, Karen E. Heath, Alexander A.L. Jorge, Tracey Kurtzman, Stephen LaFranchi, Seema Lalani, Jan Lebl, Yuezhen Lin, Evan Los, Dorothee Newbern, Catherine Nowak, Micah Olson, Jadranka PopovicStepanka Pruhova, Lenka Elblova, Jose Bernardo Quintos, Emma Segerlund, Lucia Sentchordi, Marwan Shinawi, Eva Lena Stattin, Jonathan Swartz, Ariadna Gonzalez Del Angel, Sinhue Diaz Cuellar, Hidekazu Hosono, Pedro A. Sanchez-Lara, Vivian Hwa, Jeffrey Baron, Ola Nilsson, Andrew Dauber

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Abstract

Context: Heterozygous mutations in the aggrecan gene (ACAN) cause autosomal dominant short stature with accelerated skeletal maturation. Objective: We sought to characterize the phenotypic spectrum and response to growth-promoting therapies. Patients and Methods: One hundred three individuals (57 females, 46 males) from 20 families with autosomal dominant short stature and heterozygous ACAN mutations were identified and confirmed using whole-exome sequencing, targeted next-generation sequencing, and/or Sanger sequencing. Clinical information was collected from the medical records. Results: Identified ACAN variants showed perfect cosegregation with phenotype. Adult individuals had mildly disproportionate short stature [median height, 22.8 standard deviation score (SDS); range, 25.9 to 20.9] and a history of early growth cessation. The condition was frequently associated with early-onset osteoarthritis (12 families) and intervertebral disc disease (9 families). No apparent genotype-phenotype correlation was found between the type of ACAN mutation and the presence of joint complaints. Childhood height was less affected (median height, 22.0 SDS; range, 24.2 to 20.6). Most children with ACAN mutations had advanced bone age (bone age 2 chronologic age; median, +1.3 years; range, +0.0 to +3.7 years). Nineteen individuals had received growth hormone therapy with some evidence of increased growth velocity. Conclusions: Heterozygous ACAN mutations result in a phenotypic spectrum ranging from mild and proportionate short stature to a mild skeletal dysplasia with disproportionate short stature and brachydactyly. Many affected individuals developed early-onset osteoarthritis and degenerative disc disease, suggesting dysfunction of the articular cartilage and intervertebral disc cartilage. Additional studies are needed to determine the optimal treatment strategy for these patients.

Original language	English
Pages (from-to)	460-469
Number of pages	10
Journal	Journal of Clinical Endocrinology and Metabolism
Volume	102
Issue number	2
DOIs	https://doi.org/10.1210/jc.2016-3313
State	Published - Feb 1 2017

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Gkourogianni, A., Andrew, M., Tyzinski, L., Crocker, M., Douglas, J., Dunbar, N., Fairchild, J., Funari, M. F. A., Heath, K. E., Jorge, A. A. L., Kurtzman, T., LaFranchi, S., Lalani, S., Lebl, J., Lin, Y., Los, E., Newbern, D., Nowak, C., Olson, M., ... Dauber, A. (2017). Clinical characterization of patients with autosomal dominant short stature due to aggrecan mutations. Journal of Clinical Endocrinology and Metabolism, 102(2), 460-469. https://doi.org/10.1210/jc.2016-3313

@article{4e96a9aa23f5419ea92fe1e1cbca4358,

title = "Clinical characterization of patients with autosomal dominant short stature due to aggrecan mutations",

abstract = "Context: Heterozygous mutations in the aggrecan gene (ACAN) cause autosomal dominant short stature with accelerated skeletal maturation. Objective: We sought to characterize the phenotypic spectrum and response to growth-promoting therapies. Patients and Methods: One hundred three individuals (57 females, 46 males) from 20 families with autosomal dominant short stature and heterozygous ACAN mutations were identified and confirmed using whole-exome sequencing, targeted next-generation sequencing, and/or Sanger sequencing. Clinical information was collected from the medical records. Results: Identified ACAN variants showed perfect cosegregation with phenotype. Adult individuals had mildly disproportionate short stature [median height, 22.8 standard deviation score (SDS); range, 25.9 to 20.9] and a history of early growth cessation. The condition was frequently associated with early-onset osteoarthritis (12 families) and intervertebral disc disease (9 families). No apparent genotype-phenotype correlation was found between the type of ACAN mutation and the presence of joint complaints. Childhood height was less affected (median height, 22.0 SDS; range, 24.2 to 20.6). Most children with ACAN mutations had advanced bone age (bone age 2 chronologic age; median, +1.3 years; range, +0.0 to +3.7 years). Nineteen individuals had received growth hormone therapy with some evidence of increased growth velocity. Conclusions: Heterozygous ACAN mutations result in a phenotypic spectrum ranging from mild and proportionate short stature to a mild skeletal dysplasia with disproportionate short stature and brachydactyly. Many affected individuals developed early-onset osteoarthritis and degenerative disc disease, suggesting dysfunction of the articular cartilage and intervertebral disc cartilage. Additional studies are needed to determine the optimal treatment strategy for these patients.",

author = "Alexandra Gkourogianni and Melissa Andrew and Leah Tyzinski and Melissa Crocker and Jessica Douglas and Nancy Dunbar and Jan Fairchild and Funari, {Mariana F.A.} and Heath, {Karen E.} and Jorge, {Alexander A.L.} and Tracey Kurtzman and Stephen LaFranchi and Seema Lalani and Jan Lebl and Yuezhen Lin and Evan Los and Dorothee Newbern and Catherine Nowak and Micah Olson and Jadranka Popovic and Stepanka Pruhova and Lenka Elblova and Quintos, {Jose Bernardo} and Emma Segerlund and Lucia Sentchordi and Marwan Shinawi and Stattin, {Eva Lena} and Jonathan Swartz and {Del Angel}, {Ariadna Gonzalez} and Cuellar, {Sinhue Diaz} and Hidekazu Hosono and Sanchez-Lara, {Pedro A.} and Vivian Hwa and Jeffrey Baron and Ola Nilsson and Andrew Dauber",

note = "Funding Information: The work of A.D. was supported by the Eunice Kennedy Shriver National Institute of Child Health and Human Development at the National Institutes of Health (Grant 1K23HD073351). The work of J.B. was supported by the Intramural Research Program of the Eunice Kennedy Shriver National Institute of Child Health and Human Development, National Institutes of Health. The work of O.N. And A.G. was supported by the Swedish Research Council (Grants 521-2014- 3063 and 2015-02227), the Swedish Governmental Agency for Innovation Systems (Vinnova) (Grant 2014-01438), the Marianne and Marcus Wallenberg Foundation (Grant 2014- 0096), the Stockholm County Council, the Swedish Society of Medicine, Byggm{\"a}stare Olle Engkvist's Foundation, HKH Kronprinsessan Lovisas f{\"o} rening f{\"o} r barnasjukva rd, S{\"a}llskapet Barnav ard, Stiftelsen Frimurare Barnhuset i Stockholm, and Karolinska Institutet. A.A.L.J. was supported by Grant 2013/03236-5 from the S{\~a}o Paulo Research Foundation (FAPESP), Brazil. The work of K.E.H. And L.S. was supported by grants from the Spanish Ministry of Education and Science (Grants SAF2012-30871 and SAF2015-66831-R). The work of J.L., S.P., and L.E. was supported by the Czech Health Research Council (Grant AZV 16-31211A) and the Project for Conceptual Development of Research Organization (Grant 00064203/6001), Ministry of Health, Czech Republic. Publisher Copyright: {\textcopyright} 2017 by the Endocrine Society.",

year = "2017",

month = feb,

day = "1",

doi = "10.1210/jc.2016-3313",

language = "English",

volume = "102",

pages = "460--469",

journal = "Journal of Clinical Endocrinology and Metabolism",

issn = "0021-972X",

number = "2",

}

Gkourogianni, A, Andrew, M, Tyzinski, L, Crocker, M, Douglas, J, Dunbar, N, Fairchild, J, Funari, MFA, Heath, KE, Jorge, AAL, Kurtzman, T, LaFranchi, S, Lalani, S, Lebl, J, Lin, Y, Los, E, Newbern, D, Nowak, C, Olson, M, Popovic, J, Pruhova, S, Elblova, L, Quintos, JB, Segerlund, E, Sentchordi, L, Shinawi, M, Stattin, EL, Swartz, J, Del Angel, AG, Cuellar, SD, Hosono, H, Sanchez-Lara, PA, Hwa, V, Baron, J, Nilsson, O & Dauber, A 2017, 'Clinical characterization of patients with autosomal dominant short stature due to aggrecan mutations', Journal of Clinical Endocrinology and Metabolism, vol. 102, no. 2, pp. 460-469. https://doi.org/10.1210/jc.2016-3313

TY - JOUR

T1 - Clinical characterization of patients with autosomal dominant short stature due to aggrecan mutations

AU - Gkourogianni, Alexandra

AU - Andrew, Melissa

AU - Tyzinski, Leah

AU - Crocker, Melissa

AU - Douglas, Jessica

AU - Dunbar, Nancy

AU - Fairchild, Jan

AU - Funari, Mariana F.A.

AU - Heath, Karen E.

AU - Jorge, Alexander A.L.

AU - Kurtzman, Tracey

AU - LaFranchi, Stephen

AU - Lalani, Seema

AU - Lebl, Jan

AU - Lin, Yuezhen

AU - Los, Evan

AU - Newbern, Dorothee

AU - Nowak, Catherine

AU - Olson, Micah

AU - Popovic, Jadranka

AU - Pruhova, Stepanka

AU - Elblova, Lenka

AU - Quintos, Jose Bernardo

AU - Segerlund, Emma

AU - Sentchordi, Lucia

AU - Shinawi, Marwan

AU - Stattin, Eva Lena

AU - Swartz, Jonathan

AU - Del Angel, Ariadna Gonzalez

AU - Cuellar, Sinhue Diaz

AU - Hosono, Hidekazu

AU - Sanchez-Lara, Pedro A.

AU - Hwa, Vivian

AU - Baron, Jeffrey

AU - Nilsson, Ola

AU - Dauber, Andrew

N1 - Funding Information: The work of A.D. was supported by the Eunice Kennedy Shriver National Institute of Child Health and Human Development at the National Institutes of Health (Grant 1K23HD073351). The work of J.B. was supported by the Intramural Research Program of the Eunice Kennedy Shriver National Institute of Child Health and Human Development, National Institutes of Health. The work of O.N. And A.G. was supported by the Swedish Research Council (Grants 521-2014- 3063 and 2015-02227), the Swedish Governmental Agency for Innovation Systems (Vinnova) (Grant 2014-01438), the Marianne and Marcus Wallenberg Foundation (Grant 2014- 0096), the Stockholm County Council, the Swedish Society of Medicine, Byggmästare Olle Engkvist's Foundation, HKH Kronprinsessan Lovisas fö rening fö r barnasjukva rd, Sällskapet Barnav ard, Stiftelsen Frimurare Barnhuset i Stockholm, and Karolinska Institutet. A.A.L.J. was supported by Grant 2013/03236-5 from the São Paulo Research Foundation (FAPESP), Brazil. The work of K.E.H. And L.S. was supported by grants from the Spanish Ministry of Education and Science (Grants SAF2012-30871 and SAF2015-66831-R). The work of J.L., S.P., and L.E. was supported by the Czech Health Research Council (Grant AZV 16-31211A) and the Project for Conceptual Development of Research Organization (Grant 00064203/6001), Ministry of Health, Czech Republic. Publisher Copyright: © 2017 by the Endocrine Society.

PY - 2017/2/1

Y1 - 2017/2/1

N2 - Context: Heterozygous mutations in the aggrecan gene (ACAN) cause autosomal dominant short stature with accelerated skeletal maturation. Objective: We sought to characterize the phenotypic spectrum and response to growth-promoting therapies. Patients and Methods: One hundred three individuals (57 females, 46 males) from 20 families with autosomal dominant short stature and heterozygous ACAN mutations were identified and confirmed using whole-exome sequencing, targeted next-generation sequencing, and/or Sanger sequencing. Clinical information was collected from the medical records. Results: Identified ACAN variants showed perfect cosegregation with phenotype. Adult individuals had mildly disproportionate short stature [median height, 22.8 standard deviation score (SDS); range, 25.9 to 20.9] and a history of early growth cessation. The condition was frequently associated with early-onset osteoarthritis (12 families) and intervertebral disc disease (9 families). No apparent genotype-phenotype correlation was found between the type of ACAN mutation and the presence of joint complaints. Childhood height was less affected (median height, 22.0 SDS; range, 24.2 to 20.6). Most children with ACAN mutations had advanced bone age (bone age 2 chronologic age; median, +1.3 years; range, +0.0 to +3.7 years). Nineteen individuals had received growth hormone therapy with some evidence of increased growth velocity. Conclusions: Heterozygous ACAN mutations result in a phenotypic spectrum ranging from mild and proportionate short stature to a mild skeletal dysplasia with disproportionate short stature and brachydactyly. Many affected individuals developed early-onset osteoarthritis and degenerative disc disease, suggesting dysfunction of the articular cartilage and intervertebral disc cartilage. Additional studies are needed to determine the optimal treatment strategy for these patients.

AB - Context: Heterozygous mutations in the aggrecan gene (ACAN) cause autosomal dominant short stature with accelerated skeletal maturation. Objective: We sought to characterize the phenotypic spectrum and response to growth-promoting therapies. Patients and Methods: One hundred three individuals (57 females, 46 males) from 20 families with autosomal dominant short stature and heterozygous ACAN mutations were identified and confirmed using whole-exome sequencing, targeted next-generation sequencing, and/or Sanger sequencing. Clinical information was collected from the medical records. Results: Identified ACAN variants showed perfect cosegregation with phenotype. Adult individuals had mildly disproportionate short stature [median height, 22.8 standard deviation score (SDS); range, 25.9 to 20.9] and a history of early growth cessation. The condition was frequently associated with early-onset osteoarthritis (12 families) and intervertebral disc disease (9 families). No apparent genotype-phenotype correlation was found between the type of ACAN mutation and the presence of joint complaints. Childhood height was less affected (median height, 22.0 SDS; range, 24.2 to 20.6). Most children with ACAN mutations had advanced bone age (bone age 2 chronologic age; median, +1.3 years; range, +0.0 to +3.7 years). Nineteen individuals had received growth hormone therapy with some evidence of increased growth velocity. Conclusions: Heterozygous ACAN mutations result in a phenotypic spectrum ranging from mild and proportionate short stature to a mild skeletal dysplasia with disproportionate short stature and brachydactyly. Many affected individuals developed early-onset osteoarthritis and degenerative disc disease, suggesting dysfunction of the articular cartilage and intervertebral disc cartilage. Additional studies are needed to determine the optimal treatment strategy for these patients.

UR - http://www.scopus.com/inward/record.url?scp=85012081706&partnerID=8YFLogxK

U2 - 10.1210/jc.2016-3313

DO - 10.1210/jc.2016-3313

M3 - Article

C2 - 27870580

AN - SCOPUS:85012081706

SN - 0021-972X

VL - 102

SP - 460

EP - 469

JO - Journal of Clinical Endocrinology and Metabolism

JF - Journal of Clinical Endocrinology and Metabolism

IS - 2

ER -

Clinical characterization of patients with autosomal dominant short stature due to aggrecan mutations

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