Firasat Sabika, Kaul Haiba, Ashfaq Usman Ali, Idrees Sobia
Department of Animal Sciences, Faculty of Biological Sciences, Quaid-i-Azam University, Islamabad, Pakistan.
Genetics Division, Department of Livestock Production, University of Veterinary and Animal Sciences, Ravi Campus, Pattoki, Pakistan.
Int Ophthalmol. 2018 Apr;38(2):807-814. doi: 10.1007/s10792-017-0508-4. Epub 2017 Apr 6.
The purpose of this study was to characterize the five missense mutations in CYP1B1 gene identified in Pakistani families affected with primary congenital glaucoma (PCG) using various bioinformatics and protein modeling tools.
We previously reported four novel missense mutations in CYP1B1 gene segregating in consanguineous Pakistani families. These mutations were identified by direct sequencing of all coding exons, the exon-intron boundaries and the 5' untranslated region of CYP1B1 using genomic DNA from affected and unaffected family members. In order to understand the effect of CYP1B1 mutations on protein structure and function, we used bioinformatics tools to investigate five mutations including four novels (W434R, D374E, L487P and L177R) and one known (E229K) mutation previously reported by our group in four Pakistani PCG-affected families.
In silico analysis of the missense mutations using the computational algorithms SNAP, I-Mutant 2.0 IUPred, PrDOS and PASTA predicted pathogenic effects on stability and function of protein.
In silico analysis of identified mutations confirmed their molecular pathogenicity. Similar analysis will be helpful in understanding of the biological role of CYP1B1 and the effect of mutations on the regulatory and enzymatic functions of CYP1B1 that result in PCG.
本研究的目的是使用各种生物信息学和蛋白质建模工具,对在患有原发性先天性青光眼(PCG)的巴基斯坦家庭中鉴定出的CYP1B1基因的五个错义突变进行特征描述。
我们之前报道了在近亲通婚的巴基斯坦家庭中分离出的CYP1B1基因的四个新的错义突变。这些突变是通过使用来自患病和未患病家庭成员的基因组DNA对CYP1B1的所有编码外显子、外显子-内含子边界和5'非翻译区进行直接测序来鉴定的。为了了解CYP1B1突变对蛋白质结构和功能的影响,我们使用生物信息学工具研究了五个突变,包括四个新突变(W434R、D374E、L487P和L177R)和一个我们小组之前在四个受PCG影响的巴基斯坦家庭中报道过的已知突变(E229K)。
使用计算算法SNAP、I-Mutant 2.0、IUPred、PrDOS和PASTA对错义突变进行的计算机模拟分析预测了对蛋白质稳定性和功能的致病作用。
对已鉴定突变的计算机模拟分析证实了它们的分子致病性。类似的分析将有助于理解CYP1B1的生物学作用以及突变对导致PCG的CYP1B1的调节和酶促功能的影响。
