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胸腺相关甲状旁腺激素有两种细胞来源,具有不同的内分泌和免疫功能。

Thymus-associated parathyroid hormone has two cellular origins with distinct endocrine and immunological functions.

机构信息

Department of Genetics, University of Georgia, Athens, Georgia, United States of America.

出版信息

PLoS Genet. 2010 Dec 23;6(12):e1001251. doi: 10.1371/journal.pgen.1001251.

Abstract

In mammals, parathyroid hormone (PTH) is a key regulator of extracellular calcium and inorganic phosphorus homeostasis. Although the parathyroid glands were thought to be the only source of PTH, extra-parathyroid PTH production in the thymus, which shares a common origin with parathyroids during organogenesis, has been proposed to provide an auxiliary source of PTH, resulting in a higher than expected survival rate for aparathyroid Gcm2⁻/⁻ mutants. However, the developmental ontogeny and cellular identity of these "thymic" PTH-expressing cells is unknown. We found that the lethality of aparathyroid Gcm2⁻/⁻ mutants was affected by genetic background without relation to serum PTH levels, suggesting a need to reconsider the physiological function of thymic PTH. We identified two sources of extra-parathyroid PTH in wild-type mice. Incomplete separation of the parathyroid and thymus organs during organogenesis resulted in misplaced, isolated parathyroid cells that were often attached to the thymus; this was the major source of thymic PTH in normal mice. Analysis of thymus and parathyroid organogenesis in human embryos showed a broadly similar result, indicating that these results may provide insight into human parathyroid development. In addition, medullary thymic epithelial cells (mTECs) express PTH in a Gcm2-independent manner that requires TEC differentiation and is consistent with expression as a self-antigen for negative selection. Genetic or surgical removal of the thymus indicated that thymus-derived PTH in Gcm2⁻/⁻ mutants did not provide auxiliary endocrine function. Our data show conclusively that the thymus does not serve as an auxiliary source of either serum PTH or parathyroid function. We further show that the normal process of parathyroid organogenesis in both mice and humans leads to the generation of multiple small parathyroid clusters in addition to the main parathyroid glands, that are the likely source of physiologically relevant "thymic PTH."

摘要

在哺乳动物中,甲状旁腺激素(PTH)是细胞外钙和无机磷稳态的关键调节剂。虽然甲状旁腺被认为是 PTH 的唯一来源,但胸腺中的副甲状腺 PTH 产生,在器官发生期间与甲状旁腺具有共同的起源,被认为提供了 PTH 的辅助来源,导致 aparathyroid Gcm2⁻/⁻突变体的存活率高于预期。然而,这些“胸腺”表达 PTH 的细胞的发育发生和细胞身份尚不清楚。我们发现 aparathyroid Gcm2⁻/⁻突变体的致死性受到遗传背景的影响,与血清 PTH 水平无关,这表明需要重新考虑胸腺 PTH 的生理功能。我们在野生型小鼠中发现了两种副甲状腺外 PTH 的来源。在器官发生期间,甲状旁腺和胸腺器官的不完全分离导致了错位的、孤立的甲状旁腺细胞,这些细胞经常附着在胸腺上;这是正常小鼠中胸腺 PTH 的主要来源。对人胚胎胸腺和甲状旁腺发生的分析显示了大致相似的结果,表明这些结果可能为人类甲状旁腺发育提供了一些见解。此外,髓质胸腺上皮细胞(mTEC)以 Gcm2 独立的方式表达 PTH,这需要 TEC 分化,并且与作为阴性选择的自身抗原的表达一致。胸腺的遗传或手术切除表明,在 Gcm2⁻/⁻突变体中,胸腺来源的 PTH 不能提供辅助内分泌功能。我们的数据明确表明,胸腺不能作为血清 PTH 或甲状旁腺功能的辅助来源。我们进一步表明,在小鼠和人类中,正常的甲状旁腺器官发生过程除了主要的甲状旁腺外,还会产生多个小的甲状旁腺簇,这些簇可能是生理相关的“胸腺 PTH”的来源。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e1c6/3009658/6eea7a309c4f/pgen.1001251.g001.jpg

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