肠激素在三种成骨细胞系中的受体和作用。

Q1 Biochemistry, Genetics and Molecular Biology
Elda L Pacheco-Pantoja, Lakshminarayan R Ranganath, James A Gallagher, Peter J M Wilson, William D Fraser
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引用次数: 151

摘要

背景:近年来,人们对肠道激素与骨骼过程的关系越来越感兴趣,这是骨骼研究中最有趣的方面之一。骨量与软组织的比例似乎是一种由微妙的规则控制的关系,这意味着营养摄入与脂肪等组织之间的“交叉对话”。因此,认识整合胃肠道-脂肪-骨轴的机制及其在人类健康的几个方面的应用对于改善与骨疾病相关的治疗至关重要。本研究分析了肠道激素在三种成骨细胞系细胞培养中的作用,这些细胞系代表成骨细胞发育的不同阶段。此外,这是第一次有关于胰高血糖素样肽2和肥胖抑制素对成骨细胞样细胞直接作用的报道。方法:采用逆转录和实时聚合酶链反应,分析3种成骨细胞(Saos-2、TE-85和MG-63)不同发育阶段的5种肠道激素受体(葡萄糖依赖性胰岛素肽[GIP]、胰高血糖素样肽1 [GLP-1]、胰高血糖素样肽2 [GLP-2]、生长素[GHR]和肥胖抑制素[OB]) mRNA表达水平。通过测定细胞活力和骨生化标志物:碱性磷酸酶(ALP)、前胶原1型氨基末端前肽(P1NP)和骨钙素的产生,研究了对肠道肽的反应。结果:肠激素受体mRNA在Saos-2中表达最高,在MG-63中表达最低,而GHR和GPR39(推定的肥胖抑制素受体)在TE-85和MG-63中表达较高,在Saos-2中表达较低。GLP-1和GLP-2仅在MG-63和TE-85中表达。肠道激素对细胞系的处理表现出不同的反应:GIP后Saos-2细胞活力提高,GLP-1、GLP-2、ghrelin和肥胖抑制素后TE-85和MG-63细胞活力提高。在GIP、GHR和OB后Saos-2和GHR后TE-85中ALP水平升高。Saos-2在GIP和OB后P1NP水平升高。TE-85和MG-63在GLP-1、GLP-2和OB作用后,P1NP水平下降,MG-63在GLP-2作用后骨钙素水平则相反。结论:不同营养相关肽对成骨细胞活性的调节随发育阶段的不同而不同。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Receptors and effects of gut hormones in three osteoblastic cell lines.

Receptors and effects of gut hormones in three osteoblastic cell lines.

Receptors and effects of gut hormones in three osteoblastic cell lines.

Receptors and effects of gut hormones in three osteoblastic cell lines.

Background: In recent years the interest on the relationship of gut hormones to bone processes has increased and represents one of the most interesting aspects in skeletal research. The proportion of bone mass to soft tissue is a relationship that seems to be controlled by delicate and subtle regulations that imply "cross-talks" between the nutrient intake and tissues like fat. Thus, recognition of the mechanisms that integrate a gastrointestinal-fat-bone axis and its application to several aspects of human health is vital for improving treatments related to bone diseases. This work analysed the effects of gut hormones in cell cultures of three osteoblastic cell lines which represent different stages in osteoblastic development. Also, this is the first time that there is a report on the direct effects of glucagon-like peptide 2, and obestatin on osteoblast-like cells.

Methods: mRNA expression levels of five gut hormone receptors (glucose-dependent insulinotropic peptide [GIP], glucagon-like peptide 1 [GLP-1], glucagon-like peptide 2 [GLP-2], ghrelin [GHR] and obestatin [OB]) were analysed in three osteoblastic cell lines (Saos-2, TE-85 and MG-63) showing different stages of osteoblast development using reverse transcription and real time polymerase chain reaction. The responses to the gut peptides were studied using assays for cell viability, and biochemical bone markers: alkaline phosphatase (ALP), procollagen type 1 amino-terminal propeptides (P1NP), and osteocalcin production.

Results: The gut hormone receptor mRNA displayed the highest levels for GIP in Saos-2 and the lowest levels in MG-63, whereas GHR and GPR39 (the putative obestatin receptor) expression was higher in TE-85 and MG-63 and lower in Saos-2. GLP-1 and GLP-2 were expressed only in MG-63 and TE-85. Treatment of gut hormones to cell lines showed differential responses: higher levels in cell viability in Saos-2 after GIP, in TE-85 and MG-63 after GLP-1, GLP-2, ghrelin and obestatin. ALP showed higher levels in Saos-2 after GIP, GHR and OB and in TE-85 after GHR. P1NP showed higher levels after GIP and OB in Saos-2. Decreased levels of P1NP were observed in TE-85 and MG-63 after GLP-1, GLP-2 and OB. MG-63 showed opposite responses in osteocalcin levels after GLP-2.

Conclusions: These results suggest that osteoblast activity modulation varies according to different development stage under different nutrition related-peptides.

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来源期刊
BMC Physiology
BMC Physiology Biochemistry, Genetics and Molecular Biology-Physiology
CiteScore
9.60
自引率
0.00%
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0
期刊介绍: BMC Physiology is an open access journal publishing original peer-reviewed research articles in cellular, tissue-level, organismal, functional, and developmental aspects of physiological processes. BMC Physiology (ISSN 1472-6793) is indexed/tracked/covered by PubMed, MEDLINE, BIOSIS, CAS, EMBASE, Scopus, Zoological Record and Google Scholar.
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