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The t(4;11) fusion protein MLL/AF4 regulates telomerase reverse transcriptase (TERT) expression

机译:t(4; 11)融合蛋白mLL / aF4调节端粒酶逆转录酶(TERT)表达

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摘要

The human blood consists of many different kinds of blood cells. There are the red blood cells (erythrocytes) and the white blood cells (leukocytes), further subdivided into blood cells like lymphocytes, granulocytes, monocytes etc. Those cell types have all different purposes ranging from transportation, wound healing or support of the immune system. The erythrocytes are for transportation and carry the oxygen or carbon dioxide through the blood stream. White blood cells or leukocytes include various cell types divided into four sub groups. Group one are the granulocytes containing neutrophils, eosinophils and basophils which destroy invading bacteria or parasites, secrete histamine and play a role in modulating allergic inflammation reactions. Group two consists of the monocytes which infiltrate the blood vessel surrounding tissue and differentiate to macrophages to fight pathogens or destroy damaged cells. The third group are the lymphocytes which consist of B-cells, mainly antibody producers, T-cells which play an important role in inflammation and regulating other immune cells. The last cell type in this group is the natural killer cell (NK-cell). NK cells kill virus infected cells and have been reported to kill gastric tumour cells (Miller, 2001). There are also thrombocytes in the blood which are small cell fragments produced by megakaryocytes in the bone marrow. On the other hand they support wound healing and coagulation. All of these blood cells are derived from pluripotent haematopoietic stem cells (HSC) in the bone marrow. Pluripotent stem cells create progenitor cells with a predetermined fate (Figure 1-1). HSCs are generated by a process called haematopoiesis and have been classified depending on their capacity to self-renew. In the beginning there are long-term self renewing HSCs which generate then other more short living HSCs resulting in pluripotent progenitors without self-renewal capacity (Reya et al., 2001). HSCs occupy niches in the bone marrow. A niche is a microenvironment which consists of supporting cells providing necessary cytokines for self renewal and differentiation ability (Yin and Li, 2006). 3 The differentiation process of a HSC can result in a myeloid or a lymphoid progenitor cell. Following the lineage determination a series of differentiation steps leads first to the progenitor cell and then to a precursor cell. Progenitor cells still divide at a high rate, although numbers of cell divisions are limited. Continued differentiation of the precursors finally produces the fully differentiated and mature blood cell (Alberts, 2002). In summary it can be stated that the haematopoiesis of HSCs is a delicate and a critical sequence of incidents with highly and tightly regulated processes. These processes are proliferation, maturation and differentiation. The tight regulation is necessary as for example many leukocytes are very short living and need to be replaced constantly. The half life of neutrophils in the peripheral blood for example lies between 8 and 10 hours which means there have to be ensured strictly controlled mechanisms for proper differentiation during the 10 to 14 days of their maturation. This maintains a constant level of neutrophils in the peripheral blood (Speck, 2001). Disruption of this process can lead to a disordered form of haematopoiesis called leukaemia, the cancer of the blood.
机译:人体血液由许多不同种类的血细胞组成。有红细胞(红血球)和白细胞(白血球),进一步细分为淋巴细胞,粒细胞,单核细胞等血细胞。这些细胞类型具有不同的用途,从运输,伤口愈合或支持免疫系统。红细胞用于运输,并通过血流携带氧气或二氧化碳。白细胞或白细胞包括分为四个亚组的各种细胞类型。第一组是含有嗜中性粒细胞,嗜酸性粒细胞和嗜碱性粒细胞的粒细胞,它们可破坏入侵的细菌或寄生虫,分泌组胺并在调节过敏性炎症反应中起作用。第二组由渗透到周围组织血管中的单核细胞组成,并分化为巨噬细胞以对抗病原体或破坏受损的细胞。第三类是由B细胞组成的淋巴细胞,主要是抗体产生者,T细胞在炎症和调节其他免疫细胞中起重要作用。该组中的最后一种细胞类型是自然杀伤细胞(NK细胞)。 NK细胞杀死被病毒感染的细胞,并且据报道可以杀死胃肿瘤细胞(Miller,2001)。血液中还有血小板细胞,它们是骨髓中巨核细胞产生的小细胞碎片。另一方面,它们支持伤口愈合和凝结。所有这些血细胞均来自骨髓中的多能造血干细胞(HSC)。多能干细胞产生具有预定命运的祖细胞(图1-1)。造血干细胞是由造血过程产生的,并根据其自我更新的能力进行分类。起初有长期的自我更新HSC,然后产生了其他寿命更短的HSC,导致多能祖细胞没有自我更新的能力(Reya等,2001)。 HSC占据骨髓中的适当位置。生态位是一种微环境,由支持细胞提供自我更新和分化能力所需的细胞因子组成(Yin and Li,2006)。 3 HSC的分化过程可导致髓样或淋巴样祖细胞。在谱系确定之后,一系列分化步骤首先导致祖细胞,然后导致前体细胞。尽管细胞分裂的数目受到限制,但祖细胞仍以高分裂速率分裂。前体的持续分化最终产生了完全分化和成熟的血细胞(Alberts,2002)。总之,可以说,HSC的造血作用是一系列精细而关键的事件,其过程受到高度严格的控制。这些过程是增殖,成熟和分化。严格的调节是必要的,因为例如许多白细胞的寿命很短,需要不断更换。例如,嗜中性粒细胞在外周血中的半衰期在8到10个小时之间,这意味着必须确保严格控制其成熟10到14天期间适当分化的机制。这样可以保持外周血中性粒细胞水平恒定(Speck,2001)。破坏该过程可能导致造血功能紊乱,称为白血病,即血液癌症。

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    Greßner Andreas;

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  • 年度 2011
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  • 原文格式 PDF
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