Mutations in the Human Muscle LIM Protein Gene in Families With Hypertrophic Cardiomyopathy
10.1161/01.cir.0000056522.82563.5f
Crossref journal-article
Ovid Technologies (Wolters Kluwer Health)
Circulation (276)
Abstract

Background— Muscle LIM protein (MLP) is an essential nuclear regulator of myogenic differentiation. Additionally, it may act as an integrator of protein assembly of the actin-based cytoskeleton. MLP-knockout mice develop a marked cardiac hypertrophy reaction and dilated cardiomyopathy (DCM). MLP is therefore a candidate gene for heritable forms of hypertrophic cardiomyopathy (HCM) and DCM in humans. Methods and Results— We analyzed 1100 unrelated individuals (400 patients with DCM, 200 patients with HCM, and 500 controls) for mutations in the human CRP3 gene that encodes MLP. We found 3 different missense mutations in 3 unrelated patients with familial HCM but detected no mutation in the DCM group or the controls. All mutations predicted an amino acid exchange at highly conserved residues in the functionally important LIM1 domain, which is responsible for interaction with α-actinin and with certain muscle-specific transcription factors. Protein-binding studies indicate that mutations in the CRP3 gene lead to a decreased binding activity of MLP to α-actinin. All 3 index patients were characterized by typical asymmetrical septal hypertrophy. Family studies revealed cosegregation of clinically affected individuals with the respective mutations in MLP. Conclusion— Here, we present evidence that mutations in the CRP3/MLP gene can cause HCM.

Bibliography

Geier, C., Perrot, A., Özcelik, C., Binner, P., Counsell, D., Hoffmann, K., Pilz, B., Martiniak, Y., Gehmlich, K., van der Ven, P. F. M., Fürst, D. O., Vornwald, A., von Hodenberg, E., Nürnberg, P., Scheffold, T., Dietz, R., & Osterziel, K. J. (2003). Mutations in the Human Muscle LIM Protein Gene in Families With Hypertrophic Cardiomyopathy. Circulation, 107(10), 1390–1395.

Authors 17
  1. Christian Geier (first)
  2. Andreas Perrot (additional)
  3. Cemil Özcelik (additional)
  4. Priska Binner (additional)
  5. Damian Counsell (additional)
  6. Katrin Hoffmann (additional)
  7. Bernhard Pilz (additional)
  8. Yvonne Martiniak (additional)
  9. Katja Gehmlich (additional)
  10. Peter F.M. van der Ven (additional)
  11. Dieter O. Fürst (additional)
  12. Arnold Vornwald (additional)
  13. Eberhard von Hodenberg (additional)
  14. Peter Nürnberg (additional)
  15. Thomas Scheffold (additional)
  16. Rainer Dietz (additional)
  17. Karl Josef Osterziel (additional)
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Dates
Type When
Created 22 years, 5 months ago (March 18, 2003, 6:14 a.m.)
Deposited 1 year, 3 months ago (May 6, 2024, 2:43 p.m.)
Indexed 2 weeks, 4 days ago (Aug. 19, 2025, 7:06 a.m.)
Issued 22 years, 5 months ago (March 18, 2003)
Published 22 years, 5 months ago (March 18, 2003)
Published Print 22 years, 5 months ago (March 18, 2003)
Funders 0

None

@article{Geier_2003, title={Mutations in the Human Muscle LIM Protein Gene in Families With Hypertrophic Cardiomyopathy}, volume={107}, ISSN={1524-4539}, url={http://dx.doi.org/10.1161/01.cir.0000056522.82563.5f}, DOI={10.1161/01.cir.0000056522.82563.5f}, number={10}, journal={Circulation}, publisher={Ovid Technologies (Wolters Kluwer Health)}, author={Geier, Christian and Perrot, Andreas and Özcelik, Cemil and Binner, Priska and Counsell, Damian and Hoffmann, Katrin and Pilz, Bernhard and Martiniak, Yvonne and Gehmlich, Katja and van der Ven, Peter F.M. and Fürst, Dieter O. and Vornwald, Arnold and von Hodenberg, Eberhard and Nürnberg, Peter and Scheffold, Thomas and Dietz, Rainer and Osterziel, Karl Josef}, year={2003}, month=mar, pages={1390–1395} }