Phylogenetic analysis of TET2 gene variants in Pakistani acute myeloid Leukemia patients
Mawada Elmagboul Abdalla Abakar, Mehad Almagboul Abdalla Abaker, Marco Antoniotti, Alex Graudenzi

TL;DR
This study explores TET2 gene mutations in Pakistani AML patients using phylogenetic analysis to identify population-specific patterns and potential therapeutic targets.
Contribution
The study identifies population-specific TET2 mutational hotspots and evolutionary patterns in Pakistani AML patients.
Findings
AML samples showed significant deletions in the catalytic domain of TET2, leading to reduced sequence conservation.
Phylogenetic analysis revealed distinct separation between AML and control clusters with high bootstrap values.
Findings suggest TET2 variations could inform biomarker development and targeted therapy strategies.
Abstract
Acute myeloid leukemia (AML) is a heterogeneous malignancy caused by the proliferation of neoplastic myeloid progenitor cells. With mutations in TET2 playing a critical role in leukemogenesis and therapeutic response. Population-specific mutational patterns remain largely unexplored. Multiple sequence alignment and phylogenetic analysis was used to elucidate the evolutionary conservation and divergence of TET2 sequences in Pakistani AML patients providing insights into mutational hotspots and population-specific patterns. Twenty-five TET2 gene sequences (12 AML and 13 controls) from the Pakistani population were analyzed using multiple sequence alignment, distance matrix analysis, and phylogenetic tree construction using Geneious software (https://www.geneious.com/). AML samples showed significant deletions in the catalytic domain (positions 693–876), essential for enzymatic function,…
Genes, proteins, chemicals, diseases, species, mutations and cell lines named across the full text — each resolved to its canonical identifier and authoritative record.
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Taxonomy
TopicsAcute Myeloid Leukemia Research · Protein Degradation and Inhibitors · Cancer Genomics and Diagnostics
