Association of Bone Disorder and Gene Polymorphism of PPAR-γ Pro12 Ala in Egyptian Children with β-Thalassemia

IF 0.6 Q4 HEMATOLOGY

Thalassemia Reports Pub Date : 2023-09-30 DOI:10.3390/thalassrep13040020

Ahmed M. Abdel Hamied, Heba Mostafa Ahmed, Dina H. Eldahshan, Dalia S. Morgan, Abdel Meged A. Abdel Meged, Marwa O. Elgendy, Mohamed S. Imam, Turki A. H. Alotaibi, Majed M. S. Alotaibi, Manal T. N. Alotaibi, Sarah S. S. Alshalan, Sara O. Elgendy

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Abstract

β-thalassemia is a genetic disorder affecting chromosome 16, inherited from one or both parents. In spite of the improved treatment of the hematological disorder and its complications, β-thalassemic patients still exhibit an imbalance in bone mineral turnover, resulting in diminished bone mineral density (BMD), more evident in the lumbar spine. The purpose of this study was to investigate the association between genetic polymorphism of the PPAR-γ gene and the presence of osteopenia or osteoporosis in children with β-thalassemia. This case–control study was conducted on 50 children with β-thalassemia from the pediatric hematology unit of Beni-Suef University Hospital, including 50 healthy children as the control group. The age range was 8 to 18 years. Samples of patients and control subjects were analyzed for the presence of polymorphisms of the PPAR-γ gene and other blood labs. An assay of BMD measure using dual-energy X-ray absorptiometry (DXA) was performed to investigate osteopenia or osteoporosis. Statistical analysis was used to investigate the relationship between the risk of osteopenia or osteoporosis and the presence of PPAR-γ Pro12Ala gene polymorphism. Eighteen (eleven males and seven females) of fifty patients (representing 36% of the patients group) have osteopenia with low bone mineral density (Z-score is −1 or less than 1). There was no statistically significant difference between BMD measurements in males and females. By comparing the frequency of 12 Ala gene polymorphisms between the patient group and the control group, we found that no statistically significant difference was detected. The BMD values were not significantly different between the groups of PPAR-γ Pro12Ala gene polymorphism. In conclusion, decreased BMD levels are frequent in β-thalassemia patients. PPAR-γ Pro12Ala gene polymorphism is not common in Egyptian patients with β-thalassemia. No significant relationship was found between the PPAR-γ Pro12Ala gene polymorphism and low BMD levels or osteopenia in Egyptian β-thalassemia patients. However, further studies on a larger population of Egyptian patients are needed to confirm this finding.

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埃及β-地中海贫血儿童骨疾病与PPAR-γ Pro12 α基因多态性的关系

β-地中海贫血是一种影响16号染色体的遗传性疾病，遗传自父母一方或双方。尽管血液系统疾病及其并发症的治疗有所改善，β-地中海贫血患者仍然表现出骨矿物质转换不平衡，导致骨密度(BMD)降低，在腰椎更明显。本研究的目的是探讨PPAR-γ基因多态性与β-地中海贫血儿童骨质减少或骨质疏松症之间的关系。本研究以贝尼苏夫大学附属医院儿科血液科50例β-地中海贫血患儿为研究对象，其中健康儿童50例为对照组。年龄范围为8至18岁。对患者和对照组的样本进行PPAR-γ基因和其他血液实验室的多态性分析。采用双能x线骨密度仪(DXA)测定骨密度，探讨骨质减少或骨质疏松。采用统计学方法探讨PPAR-γ Pro12Ala基因多态性与骨质疏松或骨质疏松风险的关系。50例患者中有18例(11例男性，7例女性)(占患者组的36%)骨量减少，骨密度低(Z-score为- 1或小于1)。男性和女性骨密度测量值之间无统计学差异。通过比较患者组与对照组之间12个Ala基因多态性的频率，我们发现差异无统计学意义。PPAR-γ Pro12Ala基因多态性组间骨密度值无显著差异。总之，β-地中海贫血患者经常出现骨密度下降。PPAR-γ Pro12Ala基因多态性在埃及β-地中海贫血患者中并不常见。PPAR-γ Pro12Ala基因多态性与埃及β-地中海贫血患者低骨密度或骨质减少之间无显著关系。然而，需要对更大的埃及患者群体进行进一步研究来证实这一发现。

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来源期刊

Thalassemia Reports HEMATOLOGY-

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审稿时长

10 weeks