Authors
Qianmei Zhuang, Xiaolong Liu, Meizhen Yan, Chunqiang Liu, Geng Wang, Yuying Jiang
Published in
Hemoglobin. Pages 1-8. Jul 13, 2026. Epub Jul 13, 2026.
Abstract
δβ-Thalassemia and hereditary persistence of fetal hemoglobin (HPFH) are uncommon hemoglobinopathies. This study aimed to define the molecular epidemiological features of δβ-thalassemia and HPFH in the childbearing-age population of Quanzhou, China, to inform precise prevention strategies and genetic counseling. From a free pre-pregnancy thalassemia screening cohort (n = 19,154), 92 individuals with elevated HbF (≥2%) and 11 control groups with normal HbF (≤2%) were included. DNA analysis of common deletion-type δβ-thalassemia/HPFH mutations (SEA-HPFH, Chinese type Gγ+(Aγδβ)0, Taiwan type β0) and non-deletion-type HPFH mutations was performed by gap-PCR, PCR-reverse dot hybridization, and Sanger sequencing. The correlation between hematological parameters and genotypes was also analyzed. The results suggest that the detection rate of deletion-type HPFH/δβ-thalassemia was 0.063% (12/19154), mainly SEA-HPFH and Chinese Gγ+(Aγδβ)0. The detection rate of γ-globin gene mutations and non-deletion-type HPFH was 0.329% (63/19154). 9 different γ-globin promoter mutations were identified. The most frequently detected variants were HBG2:c.-211C>T, HBG1:c.-29G>A, and HBG1:c.-272_-275dupAGCA. However, based on functional relevance, three key variants were highlighted: HBG1:c.-211C>T, HBG1:c.-249C>T, and the novel HBG2:c.-253_-254dup. The remaining variants (HBG1:c.-29G>A, HBG1:c.-272_-275dupAGCA, HBG1:c.-404A>G, HBG1:c.-417G>C, HBG1:c.-420C>A) are described as benign polymorphisms or variants in strong linkage disequilibrium with HBG2:c.-211C>T. Deletion-type δβ-thalassemia/HPFH is rare in Quanzhou. SEA-HPFH and Chinese Gγ+(Aγδβ)0 are more common. Non-deletion-type HPFH, especially the double heterozygous state HBG1:c.-29G>A/HBG2:c.-211C>T, is significantly more common. These findings reveal the unique molecular epidemiological characteristics of δβ-thalassemia and HPFH in this region, providing important data for genetic counseling and prenatal diagnosis.
PMID:
42443740
Bibliographic data and abstract were imported from PubMed on 14 Jul 2026.
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