PTRH2 Gene Variants: Recent Review of the Phenotypic Features and Their Bioinformatics Analysis

Rajech Sharkia; Sahil Jain; Muhammad Mahajnah; Clair Habib; Abdussalam Azem; Wasif Al-Shareef; Abdelnaser Zalan

doi:10.3390/genes14051031

PTRH2 Gene Variants: Recent Review of the Phenotypic Features and Their Bioinformatics Analysis

Genes (Basel). 2023 Apr 30;14(5):1031. doi: 10.3390/genes14051031.

Authors

Rajech Sharkia^{1

2}, Sahil Jain³, Muhammad Mahajnah^{4

5}, Clair Habib⁶, Abdussalam Azem³, Wasif Al-Shareef¹, Abdelnaser Zalan¹

Affiliations

¹ Unit of Human Biology and Genetics, Triangle Regional Research and Development Center, Kfar Qari 30075, Israel.
² Unit of Natural Sciences, Beit-Berl Academic College, Beit-Berl 4490500, Israel.
³ Department of Biochemistry and Molecular Biology, Faculty of Life Sciences, Tel Aviv University, Tel Aviv 69978, Israel.
⁴ The Ruth and Bruce Rappaport Faculty of Medicine, Technion-Israel Institute of Technology, Haifa 31096, Israel.
⁵ Child Neurology and Development Center, Hillel Yaffe Medical Center, Hadera 38100, Israel.
⁶ Genetics Institute, Rambam Health Care Campus, Haifa 31096, Israel.

Abstract

Peptidyl-tRNA hydrolase 2 (PTRH2) is an evolutionarily highly conserved mitochondrial protein. The biallelic mutations in the PTRH2 gene have been suggested to cause a rare autosomal recessive disorder characterized by an infantile-onset multisystem neurologic endocrine and pancreatic disease (IMNEPD). Patients with IMNEPD present varying clinical manifestations, including global developmental delay associated with microcephaly, growth retardation, progressive ataxia, distal muscle weakness with ankle contractures, demyelinating sensorimotor neuropathy, sensorineural hearing loss, and abnormalities of thyroid, pancreas, and liver. In the current study, we conducted an extensive literature review with an emphasis on the variable clinical spectrum and genotypes in patients. Additionally, we reported on a new case with a previously documented mutation. A bioinformatics analysis of the various PTRH2 gene variants was also carried out from a structural perspective. It appears that the most common clinical characteristics among all patients include motor delay (92%), neuropathy (90%), distal weakness (86.4%), intellectual disability (84%), hearing impairment (80%), ataxia (79%), and deformity of head and face (~70%). The less common characteristics include hand deformity (64%), cerebellar atrophy/hypoplasia (47%), and pancreatic abnormality (35%), while the least common appear to be diabetes mellitus (~30%), liver abnormality (~22%), and hypothyroidism (16%). Three missense mutations were revealed in the PTRH2 gene, the most common one being Q85P, which was shared by four different Arab communities and was presented in our new case. Moreover, four different nonsense mutations in the PTRH2 gene were detected. It may be concluded that disease severity depends on the PTRH2 gene variant, as most of the clinical features are manifested by nonsense mutations, while only the common features are presented by missense mutations. A bioinformatics analysis of the various PTRH2 gene variants also suggested the mutations to be deleterious, as they seem to disrupt the structural confirmation of the enzyme, leading to loss of stability and functionality.

Keywords: IMNEPD; PTRH2 gene; PTRH2 variants; autosomal recessive disorder; bioinformatics analysis; clinical features; rare genetic diseases.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Ataxia
Carboxylic Ester Hydrolases* / genetics
Cerebellar Ataxia* / genetics
Codon, Nonsense
Humans
Mitochondrial Proteins* / genetics
Mutation
Nervous System Malformations* / genetics

Substances

Codon, Nonsense
PTH2 protein, human
Carboxylic Ester Hydrolases
Mitochondrial Proteins

Supplementary concepts

Cerebellar Hypoplasia

Grants and funding

This study was supported by limited internal resources from the Triangle Research and Development Center (TRDC).