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马来西亚健康人和β地中海贫血患者血红蛋白在伯乐Variant II CE-HPLC早期洗脱峰中α、β、γ和δ珠蛋白链的相对蛋白质组定量分析

Relative proteome quantification of alpha, beta, gamma and delta globin chains in early eluting peaks of Bio-Rad variant II CE-HPLC of hemoglobin from healthy and beta-thalassemia subjects in Malaysia.

作者信息

Abdullah Uday Younis Hussein, Ibrahim Hishamshah M, Jassim Haitham Muhammed, Salleh Mohamad Zaki, Kek Teh Lay, Fakhruzzaman Bin Noorizhab Mohd Nur, Zilfalil Bin Alwi, Wilairat Prapin, Fucharoen Suthat

机构信息

Faculty of Medicine, Universiti Sultan Zainal Abidin, Medical Campus, 20400, Kuala Terengganu, Terengganu, Malaysia.

Paediatric Department, Hospital Kuala Lumpur (HKL), Jalan Pahang, 50586, Kuala Lumpur, Malaysia.

出版信息

Biochem Biophys Rep. 2019 Apr 28;18:100635. doi: 10.1016/j.bbrep.2019.100635. eCollection 2019 Jul.

Abstract

This is the first report of QQQ-mass spectrometric identification and quantification of the Hb subunits, alpha, beta, delta and gamma globin peptides, derived from enzymatic-digestion of proteins in the early unknown peaks of the Bio-Rad cation-exchange chromatography of haemoglobin. The objectives were to assess the relationship of the quantity of the free alpha, beta, delta and gamma globin chains with the phenotypic diversity of beta-thalassaemias (β-thal). The results demonstrate that the pools of free globin chains in red blood cells were correlating with the severity of the disease in patients with different phenotypes of β-thal. The mechanism and the regulation of synthesis of free globin chains pool in a normal individual and in patients with different β-thal phenotypes could arise from several mechanisms which will require further investigation. The role of the free globin pool in patients with β-thal for development of novel therapeutic approaches based on these potential targets requires further investigation. Pertinent biomarkers improves the diagnosis of the β-thal, especially in low-income countries where they are most common and allows more effective therapeutic intervention leading to more successful therapeutic outcome.

摘要

这是关于通过串联四极杆质谱法鉴定和定量血红蛋白亚基(α、β、δ和γ珠蛋白肽)的首份报告,这些亚基肽源自血红蛋白在伯乐阳离子交换色谱早期未知峰中蛋白质的酶解。目的是评估游离α、β、δ和γ珠蛋白链的数量与β地中海贫血(β-地贫)表型多样性之间的关系。结果表明,红细胞中游离珠蛋白链库与不同表型β-地贫患者的疾病严重程度相关。正常个体和不同β-地贫表型患者中游离珠蛋白链库的合成机制和调控可能源于多种机制,这需要进一步研究。游离珠蛋白库在β-地贫患者中基于这些潜在靶点开发新型治疗方法的作用也需要进一步研究。相关生物标志物可改善β-地贫的诊断,尤其是在其最为常见的低收入国家,并能实现更有效的治疗干预,从而带来更成功的治疗结果。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8498/6488526/2b929ea2020d/gr1a.jpg

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