Molecular characterization and investigation of the role of genetic variation in phenotypic variability and response to treatment in a large pediatric Marfan syndrome cohort

Josephina A.N. Meester; Silke Peeters; Lotte Van Den Heuvel; Geert Vandeweyer; Erik Fransen; Elizabeth Cappella; Harry C. Dietz; Geoffrey Forbus; Bruce D. Gelb; Elizabeth Goldmuntz; Arvind Hoskoppal; Andrew P. Landstrom; Teresa Lee; Seema Mital; Shaine Morris; Aaron K. Olson; Marjolijn Renard; Dan M. Roden; Michael N. Singh; Elif Seda Selamet Tierney; Justin T. Tretter; Sara L. Van Driest; Marcia Willing; Aline Verstraeten; Lut Van Laer; Ronald V. Lacro; Bart L. Loeys

doi:10.1016/j.gim.2021.12.015

Molecular characterization and investigation of the role of genetic variation in phenotypic variability and response to treatment in a large pediatric Marfan syndrome cohort

Josephina A.N. Meester, Silke Peeters, Lotte Van Den Heuvel, Geert Vandeweyer, Erik Fransen, Elizabeth Cappella, Harry C. Dietz, Geoffrey Forbus, Bruce D. Gelb, Elizabeth Goldmuntz, Arvind Hoskoppal, Andrew P. Landstrom, Teresa Lee, Seema Mital, Shaine Morris, Aaron K. Olson, Marjolijn Renard, Dan M. Roden, Michael N. Singh, Elif Seda Selamet TierneyJustin T. Tretter, Sara L. Van Driest, Marcia Willing, Aline Verstraeten, Lut Van Laer, Ronald V. Lacro, Bart L. Loeys

School of Medicine

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

Abstract

Purpose: In a large cohort of 373 pediatric patients with Marfan syndrome (MFS) with a severe cardiovascular phenotype, we explored the proportion of patients with MFS with a pathogenic FBN1 variant and analyzed whether the type/location of FBN1 variants was associated with specific clinical characteristics and response to treatment. Patients were recruited on the basis of the following criteria: aortic root z-score > 3, age 6 months to 25 years, no prior or planned surgery, and aortic root diameter < 5 cm. Methods: Targeted resequencing and deletion/duplication testing of FBN1 and related genes were performed. Results: We identified (likely) pathogenic FBN1 variants in 91% of patients. Ectopia lentis was more frequent in patients with dominant-negative (DN) variants (61%) than in those with haploinsufficient variants (27%). For DN FBN1 variants, the prevalence of ectopia lentis was highest in the N-terminal region (84%) and lowest in the C-terminal region (17%). The association with a more severe cardiovascular phenotype was not restricted to DN variants in the neonatal FBN1 region (exon 25-33) but was also seen in the variants in exons 26 to 49. No difference in the therapeutic response was detected between genotypes. Conclusion: Important novel genotype–phenotype associations involving both cardiovascular and extra-cardiovascular manifestations were identified, and existing ones were confirmed. These findings have implications for prognostic counseling of families with MFS.

Original language	English (US)
Pages (from-to)	1045-1053
Number of pages	9
Journal	Genetics in Medicine
Volume	24
Issue number	5
DOIs	https://doi.org/10.1016/j.gim.2021.12.015
State	Published - May 2022

Keywords

Clinical genetics
Connective tissue disease
FBN1
Genotype–phenotype associations
Marfan syndrome

ASJC Scopus subject areas

Genetics(clinical)

Access to Document

10.1016/j.gim.2021.12.015

Cite this

Meester, J. A. N., Peeters, S., Van Den Heuvel, L., Vandeweyer, G., Fransen, E., Cappella, E., Dietz, H. C., Forbus, G., Gelb, B. D., Goldmuntz, E., Hoskoppal, A., Landstrom, A. P., Lee, T., Mital, S., Morris, S., Olson, A. K., Renard, M., Roden, D. M., Singh, M. N., ... Loeys, B. L. (2022). Molecular characterization and investigation of the role of genetic variation in phenotypic variability and response to treatment in a large pediatric Marfan syndrome cohort. Genetics in Medicine, 24(5), 1045-1053. https://doi.org/10.1016/j.gim.2021.12.015

Molecular characterization and investigation of the role of genetic variation in phenotypic variability and response to treatment in a large pediatric Marfan syndrome cohort. / Meester, Josephina A.N.; Peeters, Silke; Van Den Heuvel, Lotte et al.
In: Genetics in Medicine, Vol. 24, No. 5, 05.2022, p. 1045-1053.

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

Meester, JAN, Peeters, S, Van Den Heuvel, L, Vandeweyer, G, Fransen, E, Cappella, E, Dietz, HC, Forbus, G, Gelb, BD, Goldmuntz, E, Hoskoppal, A, Landstrom, AP, Lee, T, Mital, S, Morris, S, Olson, AK, Renard, M, Roden, DM, Singh, MN, Selamet Tierney, ES, Tretter, JT, Van Driest, SL, Willing, M, Verstraeten, A, Van Laer, L, Lacro, RV & Loeys, BL 2022, 'Molecular characterization and investigation of the role of genetic variation in phenotypic variability and response to treatment in a large pediatric Marfan syndrome cohort', Genetics in Medicine, vol. 24, no. 5, pp. 1045-1053. https://doi.org/10.1016/j.gim.2021.12.015

@article{d617db481f58452492bc5045bd78cd99,

title = "Molecular characterization and investigation of the role of genetic variation in phenotypic variability and response to treatment in a large pediatric Marfan syndrome cohort",

abstract = "Purpose: In a large cohort of 373 pediatric patients with Marfan syndrome (MFS) with a severe cardiovascular phenotype, we explored the proportion of patients with MFS with a pathogenic FBN1 variant and analyzed whether the type/location of FBN1 variants was associated with specific clinical characteristics and response to treatment. Patients were recruited on the basis of the following criteria: aortic root z-score > 3, age 6 months to 25 years, no prior or planned surgery, and aortic root diameter < 5 cm. Methods: Targeted resequencing and deletion/duplication testing of FBN1 and related genes were performed. Results: We identified (likely) pathogenic FBN1 variants in 91% of patients. Ectopia lentis was more frequent in patients with dominant-negative (DN) variants (61%) than in those with haploinsufficient variants (27%). For DN FBN1 variants, the prevalence of ectopia lentis was highest in the N-terminal region (84%) and lowest in the C-terminal region (17%). The association with a more severe cardiovascular phenotype was not restricted to DN variants in the neonatal FBN1 region (exon 25-33) but was also seen in the variants in exons 26 to 49. No difference in the therapeutic response was detected between genotypes. Conclusion: Important novel genotype–phenotype associations involving both cardiovascular and extra-cardiovascular manifestations were identified, and existing ones were confirmed. These findings have implications for prognostic counseling of families with MFS.",

keywords = "Clinical genetics, Connective tissue disease, FBN1, Genotype–phenotype associations, Marfan syndrome",

author = "Meester, {Josephina A.N.} and Silke Peeters and {Van Den Heuvel}, Lotte and Geert Vandeweyer and Erik Fransen and Elizabeth Cappella and Dietz, {Harry C.} and Geoffrey Forbus and Gelb, {Bruce D.} and Elizabeth Goldmuntz and Arvind Hoskoppal and Landstrom, {Andrew P.} and Teresa Lee and Seema Mital and Shaine Morris and Olson, {Aaron K.} and Marjolijn Renard and Roden, {Dan M.} and Singh, {Michael N.} and {Selamet Tierney}, {Elif Seda} and Tretter, {Justin T.} and {Van Driest}, {Sara L.} and Marcia Willing and Aline Verstraeten and {Van Laer}, Lut and Lacro, {Ronald V.} and Loeys, {Bart L.}",

note = "Publisher Copyright: {\textcopyright} 2021 The Authors",

year = "2022",

month = may,

doi = "10.1016/j.gim.2021.12.015",

language = "English (US)",

volume = "24",

pages = "1045--1053",

journal = "Genetics in Medicine",

issn = "1098-3600",

publisher = "Elsevier B.V.",

number = "5",

}

TY - JOUR

T1 - Molecular characterization and investigation of the role of genetic variation in phenotypic variability and response to treatment in a large pediatric Marfan syndrome cohort

AU - Meester, Josephina A.N.

AU - Peeters, Silke

AU - Van Den Heuvel, Lotte

AU - Vandeweyer, Geert

AU - Fransen, Erik

AU - Cappella, Elizabeth

AU - Dietz, Harry C.

AU - Forbus, Geoffrey

AU - Gelb, Bruce D.

AU - Goldmuntz, Elizabeth

AU - Hoskoppal, Arvind

AU - Landstrom, Andrew P.

AU - Lee, Teresa

AU - Mital, Seema

AU - Morris, Shaine

AU - Olson, Aaron K.

AU - Renard, Marjolijn

AU - Roden, Dan M.

AU - Singh, Michael N.

AU - Selamet Tierney, Elif Seda

AU - Tretter, Justin T.

AU - Van Driest, Sara L.

AU - Willing, Marcia

AU - Verstraeten, Aline

AU - Van Laer, Lut

AU - Lacro, Ronald V.

AU - Loeys, Bart L.

PY - 2022/5

Y1 - 2022/5

N2 - Purpose: In a large cohort of 373 pediatric patients with Marfan syndrome (MFS) with a severe cardiovascular phenotype, we explored the proportion of patients with MFS with a pathogenic FBN1 variant and analyzed whether the type/location of FBN1 variants was associated with specific clinical characteristics and response to treatment. Patients were recruited on the basis of the following criteria: aortic root z-score > 3, age 6 months to 25 years, no prior or planned surgery, and aortic root diameter < 5 cm. Methods: Targeted resequencing and deletion/duplication testing of FBN1 and related genes were performed. Results: We identified (likely) pathogenic FBN1 variants in 91% of patients. Ectopia lentis was more frequent in patients with dominant-negative (DN) variants (61%) than in those with haploinsufficient variants (27%). For DN FBN1 variants, the prevalence of ectopia lentis was highest in the N-terminal region (84%) and lowest in the C-terminal region (17%). The association with a more severe cardiovascular phenotype was not restricted to DN variants in the neonatal FBN1 region (exon 25-33) but was also seen in the variants in exons 26 to 49. No difference in the therapeutic response was detected between genotypes. Conclusion: Important novel genotype–phenotype associations involving both cardiovascular and extra-cardiovascular manifestations were identified, and existing ones were confirmed. These findings have implications for prognostic counseling of families with MFS.

AB - Purpose: In a large cohort of 373 pediatric patients with Marfan syndrome (MFS) with a severe cardiovascular phenotype, we explored the proportion of patients with MFS with a pathogenic FBN1 variant and analyzed whether the type/location of FBN1 variants was associated with specific clinical characteristics and response to treatment. Patients were recruited on the basis of the following criteria: aortic root z-score > 3, age 6 months to 25 years, no prior or planned surgery, and aortic root diameter < 5 cm. Methods: Targeted resequencing and deletion/duplication testing of FBN1 and related genes were performed. Results: We identified (likely) pathogenic FBN1 variants in 91% of patients. Ectopia lentis was more frequent in patients with dominant-negative (DN) variants (61%) than in those with haploinsufficient variants (27%). For DN FBN1 variants, the prevalence of ectopia lentis was highest in the N-terminal region (84%) and lowest in the C-terminal region (17%). The association with a more severe cardiovascular phenotype was not restricted to DN variants in the neonatal FBN1 region (exon 25-33) but was also seen in the variants in exons 26 to 49. No difference in the therapeutic response was detected between genotypes. Conclusion: Important novel genotype–phenotype associations involving both cardiovascular and extra-cardiovascular manifestations were identified, and existing ones were confirmed. These findings have implications for prognostic counseling of families with MFS.

KW - Clinical genetics

KW - Connective tissue disease

KW - FBN1

KW - Genotype–phenotype associations

KW - Marfan syndrome

UR - http://www.scopus.com/inward/record.url?scp=85122993519&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=85122993519&partnerID=8YFLogxK

U2 - 10.1016/j.gim.2021.12.015

DO - 10.1016/j.gim.2021.12.015

M3 - Article

C2 - 35058154

AN - SCOPUS:85122993519

SN - 1098-3600

VL - 24

SP - 1045

EP - 1053

JO - Genetics in Medicine

JF - Genetics in Medicine

IS - 5

ER -

Molecular characterization and investigation of the role of genetic variation in phenotypic variability and response to treatment in a large pediatric Marfan syndrome cohort

Abstract

Keywords

ASJC Scopus subject areas

Access to Document

Other files and links

Fingerprint

Cite this