Clinical and genetic investigation of 14 families with various forms of short stature syndromes.

Fati Ullah Khan,Fatima Bibi,Shabir Hussain,Muhammad Javed Khan,Muhammad Ansar,Imran Ullah,Inam Ullah Khan,Tooba Hanif,Muhammad Bilal,Weizhen Ji,Zamrud Zehri,Muhammad Zahid,Abdullah Abdullah,Sohail Ahmed,Gul Hassan,Raza Sufyan,Hamid Ali,Tobias B Haack,Wasim Ahmad,Outi Mikitie,Outi Mikitie,Saquib A Lakhani,Khadim Shah,Khadim Shah,Kifayat Ullah,Shabir Hussain,Rebecca Buchert,Hammal Khan,Abdullah Abdullah,Farooq Ahmad,Raja Hussain Ali,Outi Mikitie,Faisal Faisal,Muhammad Bilal,Hammal Khan,Amjad Ali,Raja Hussain Ali,Amir Hayat,Muhammad Ilyas,Shoaib Nawaz,Rehmat Ullah,Khurrum Liaqat,Aamir Sohail,Susana Peralta,Maria Hayat,Outi Mikitie,Shoaib Nawaz,Muhammad Sharif Hasni

doi:10.1111/cge.14550

Abstract

Skeletal dysplasias are a heterogeneous group of disorders presenting mild to lethal defects. Several factors, such as genetic, prenatal, and postnatal environmental may contribute to reduced growth. Fourteen families of Pakistani origin, presenting the syndromic form of short stature either in the autosomal recessive or autosomal dominant manner were clinically and genetically investigated to uncover the underlying genetic etiology. Homozygosity mapping, whole exome sequencing, and Sanger sequencing were used to search for the disease-causing gene variants. In total, we have identified 13 sequence variants in 10 different genes. The variants in the HSPG2 and XRCC4 genes were not reported previously in the Pakistani population. This study will expand the mutation spectrum of the identified genes and will help in improved diagnosis of the syndromic form of short stature in the local population.

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