Identities and frequencies of variants in CYP1B1 causing primary congenital glaucoma in Pakistan

Muhammad Rashid; Sairah Yousaf; Shakeel A. Sheikh; Zureesha Sajid; Asra S. Shabbir; Tasleem Kausar; Nabeela Tariq; Muhammad Usman; Rehan S. Shaikh; Muhammad Ali; Shazia A. Bukhari; Ali M. Waryah; Muhammad Qasim; Saima Riazuddin; Zubair M. Ahmed

Molecular Vision (Feb 2019)

Identities and frequencies of variants in CYP1B1 causing primary congenital glaucoma in Pakistan

Muhammad Rashid,
Sairah Yousaf,
Shakeel A. Sheikh,
Zureesha Sajid,
Asra S. Shabbir,
Tasleem Kausar,
Nabeela Tariq,
Muhammad Usman,
Rehan S. Shaikh,
Muhammad Ali,
Shazia A. Bukhari,
Ali M. Waryah,
Muhammad Qasim,
Saima Riazuddin,
Zubair M. Ahmed

Affiliations

Muhammad Rashid: Department of Otorhinolaryngology Head and Neck Surgery, School of Medicine, University of Maryland, Baltimore, MD; Department of Bioinformatics and Biotechnology, Government College University, Faisalabad, Pakistan
Sairah Yousaf: Department of Otorhinolaryngology Head and Neck Surgery, School of Medicine, University of Maryland, Baltimore, MD
Shakeel A. Sheikh: Molecular Biology & Genetics Department, Liaquat University of Medical & Health Sciences, Jamshoro, Pakistan
Zureesha Sajid: Department of Otorhinolaryngology Head and Neck Surgery, School of Medicine, University of Maryland, Baltimore, MD; Institute of Molecular Biology & Biotechnology, Bahauddin Zakariya University, Multan, Pakistan
Asra S. Shabbir: University College of Pharmacy, Punjab University, Lahore, Pakistan
Tasleem Kausar: Zoology Department, Government Sadiq College Women University, Bahawalpur, Pakistan
Nabeela Tariq: Zoology Department, Sardar Bahadur Khan Women University, Quetta, Pakistan
Muhammad Usman: Department of Bioinformatics and Biotechnology, Government College University, Faisalabad, Pakistan
Rehan S. Shaikh: Institute of Molecular Biology & Biotechnology, Bahauddin Zakariya University, Multan, Pakistan
Muhammad Ali: Department of Biochemistry, Government College University, Faisalabad, Pakistan
Shazia A. Bukhari: Department of Biochemistry, Government College University, Faisalabad, Pakistan
Ali M. Waryah: Molecular Biology & Genetics Department, Liaquat University of Medical & Health Sciences, Jamshoro, Pakistan
Muhammad Qasim: Department of Bioinformatics and Biotechnology, Government College University, Faisalabad, Pakistan
Saima Riazuddin: Department of Otorhinolaryngology Head and Neck Surgery, School of Medicine, University of Maryland, Baltimore, MD
Zubair M. Ahmed: Department of Otorhinolaryngology Head and Neck Surgery, School of Medicine, University of Maryland, Baltimore, MD

Journal volume & issue: Vol. 25, no. 1
pp. 144 – 154

Abstract

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Purpose: Primary congenital glaucoma (PCG) is a clinically and genetically heterogeneous disease. The present study was undertaken to find the genetic causes of PCG segregating in 36 large consanguineous Pakistani families. Methods: Ophthalmic examination including fundoscopy, or slit-lamp microscopy was performed to clinically characterize the PCG phenotype. Genomic nucleotide sequences of the CYP1B1 and LTBP2 genes were analyzed with either Sanger or whole exome sequencing. In silico prediction programs were used to assess the pathogenicity of identified alleles. ClustalW alignments were performed to determine evolutionary conservation, and three-dimensional (3D) modeling was performed using HOPE and Phyre2 software. Results: Among the known loci, mutations in CYP1B1 and LTBP2 are the common causes of PCG. Therefore, we analyzed the genomic nucleotide sequences of CYP1B1 and LTBP2, and detected probable pathogenic variants cosegregating with PCG in 14 families. These included the three novel (c.542T>A, c.1436A>G, and c.1325delC) and five known (c.868dupC, c.1168C>T, c.1169G>A, c.1209InsTCATGCCACC, and c.1310C>T) variants in CYP1B1. Two of the novel variants are missense substitutions [p.(Leu181Gln), p.(Gln479Arg)], which replaced evolutionary conserved amino acids, and are predicted to be pathogenic by various in silico programs, while the third variant (c.1325delC) is predicted to cause reading frameshift and premature truncation of the protein. A single mutation, p.(Arg390His), causes PCG in six (~43%) of the 14 CYP1B1 mutations harboring families, and thus, is the most common variant in this cohort. Surprisingly, we did not find any LTBP2 pathogenic variants in the families, which further supports the genetic heterogeneity of PCG in the Pakistani population. Conclusions: In conclusion, results of the present study enhance our understanding of the genetic basis of PCG, support the notion of a genetic modifier of CYP1B1, and contribute to the development of genetic testing protocols and genetic counseling for PCG in Pakistani families.

Published in Molecular Vision

ISSN: 1090-0535 (Online)
Publisher: Molecular Vision
Country of publisher: United States
LCC subjects: Science: Biology (General): Genetics
Website: http://www.molvis.org/molvis/

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