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血浆凝胶蛋白在红细胞生成的终末阶段及体外纠正红细胞发育异常中的作用。

Role of Plasma Gelsolin Protein in the Final Stage of Erythropoiesis and in Correction of Erythroid Dysplasia In Vitro.

机构信息

Department of Laboratory Medicine, College of Medicine, Hanyang University, Seoul 04763, Korea.

Department of Translational Medicine, Graduate School of Biomedical Science and Engineering, Hanyang University, Seoul 04763, Korea.

出版信息

Int J Mol Sci. 2020 Sep 27;21(19):7132. doi: 10.3390/ijms21197132.

Abstract

Gelsolin, an actin-remodeling protein, is involved in cell motility, cytoskeletal remodeling, and cytokinesis and is abnormally expressed in many cancers. Recently, human recombinant plasma gelsolin protein (pGSN) was reported to have important roles in cell cycle and maturation of primary erythroblasts. However, the role of human plasma gelsolin in late stage erythroblasts prior to enucleation and putative clinical relevance in patients with myelodysplastic syndrome (MDS) and hemato-oncologic diseases have not been reported. Polychromatic and orthochromatic erythroblasts differentiated from human cord blood CD34+ cells, and human bone marrow (BM) cells derived from patients with MDS, were cultured in serum-free medium containing pGSN. Effects of pGSN on mitochondria, erythroid dysplasia, and enucleation were assessed in cellular and transcriptional levels. With pGSN treatment, terminal maturation at the stage of poly- and ortho-chromatic erythroblasts was enhanced, with higher numbers of orthochromatic erythroblasts and enucleated red blood cells (RBCs). pGSN also significantly decreased dysplastic features of cell morphology. Moreover, we found that patients with MDS with multi-lineage dysplasia or with excess blasts-1 showed significantly decreased expression of gelsolin mRNA () in their peripheral blood. When BM erythroblasts of MDS patients were cultured with pGSN, levels of mRNA transcripts related to terminal erythropoiesis and enucleation were markedly increased, with significantly decreased erythroid dysplasia. Moreover, pGSN treatment enhanced mitochondrial transmembrane potential that is unregulated in MDS and cultured cells. Our findings demonstrate a key role for plasma gelsolin in erythropoiesis and in gelsolin-depleted MDS patients, and raises the possibility that pGSN administration may promote erythropoiesis in erythroid dysplasia.

摘要

肌动蛋白重塑蛋白凝胶蛋白参与细胞运动、细胞骨架重塑和胞质分裂,在许多癌症中异常表达。最近,人重组血浆凝胶蛋白(pGSN)被报道在原红细胞的细胞周期和成熟中具有重要作用。然而,人血浆凝胶蛋白在去核前的晚期红细胞中的作用以及在骨髓增生异常综合征(MDS)和血液肿瘤疾病患者中的潜在临床相关性尚未报道。从人脐血 CD34+细胞和 MDS 患者骨髓中分化的多色性和正染红细胞在含 pGSN 的无血清培养基中培养。在细胞和转录水平评估 pGSN 对线粒体、红细胞发育不良和去核的影响。用 pGSN 处理后,多色性和正染红细胞阶段的终末成熟增强,正染红细胞和去核的红细胞(RBC)数量增加。pGSN 还显著降低了细胞形态的发育不良特征。此外,我们发现具有多谱系发育不良或有过多原始细胞-1 的 MDS 患者其外周血中的凝胶蛋白 mRNA 表达显著降低()。当 MDS 患者的 BM 红细胞用 pGSN 培养时,与终末红细胞生成和去核相关的 mRNA 转录本水平显著增加,红细胞发育不良明显减少。此外,pGSN 处理增强了 MDS 中未调节的线粒体跨膜电位和培养细胞。我们的研究结果表明,血浆凝胶蛋白在红细胞生成和凝胶蛋白耗竭的 MDS 患者中起着关键作用,并提出了 pGSN 给药可能促进红细胞发育不良中的红细胞生成的可能性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/eb89/7583768/6e231be8d3d5/ijms-21-07132-g001.jpg

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