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Lysosomal storage disorders - challenges, concepts and avenues for therapy: beyond rare diseases

机译:溶酶体储存障碍 - 治疗的挑战,概念和途径:超越稀有疾病

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摘要

The pivotal role of lysosomes in cellular processes is increasingly appreciated. An understanding of the balanced interplay between the activity of acidic hydrolases, lysosomal membrane proteins and cytosolic proteins is required. Lysosomal storage diseases (LSDs) are characterized by disturbances in this network and by intralysosomal accumulation of substrates, often only in certain cell types. Even though our knowledge of these diseases has increased and therapies have been established, many aspects of the molecular pathology of LSDs remain obscure. This Review aims to discuss how lysosomal storage affects functions linked to lysosomes, such as membrane repair, autophagy, exocytosis, lipid homeostasis, signalling cascades and cell viability. Therapies must aim to correct lysosomal storage not only morphologically, but reverse its (patho)biochemical consequences. As different LSDs have different molecular causes, this requires custom tailoring of therapies. We will discuss the major advantages and drawbacks of current and possible future therapies for LSDs. Study of the pathological molecular mechanisms underlying these 'experiments of nature' often yields information that is relevant for other conditions found in the general population. Therefore, more common diseases may profit from a correction of impaired lysosomal function.
机译:溶酶体在细胞过程中的关键作用越来越高兴。需要了解酸性水解酶,溶酶体膜蛋白和细胞溶质蛋白的活性之间的平衡相互作用。溶酶体储存疾病(LSDS)的特征在于该网络中的干扰以及血管内血管基质积累,通常仅在某些细胞类型中。尽管我们对这些疾病的知识增加了增加和疗法,但LSD的分子病理学的许多方面仍然模糊不清。该审查旨在讨论溶酶体储存如何影响与溶酶体相关的功能,例如膜修复,自噬,外尿精,脂质稳态,信号级联和细胞活力。疗法必须旨在纠正溶酶体储存不仅是形态学,而且逆转其生物化学后果。随着不同的LSD具有不同的分子原因,这需要定制疗法剪裁。我们将讨论LSD的当前和可能的未来疗法的主要优势和缺点。这些“自然实验”潜在的病理分子机制的研究通常会产生与一般人群中的其他条件相关的信息。因此,更常见的疾病可能从溶酶体功能受损的校正中获利。

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