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Review
. 2009 Feb 1;8(3):391-3.
doi: 10.4161/cc.8.3.7545. Epub 2009 Feb 4.

VSports最新版本 - Autophagy in mineralizing tissues: microenvironmental perspectives

Vickram Srinivas  1 Jolene BohenskyAdam M ZahmIrving M Shapiro
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Review

Autophagy in mineralizing tissues: microenvironmental perspectives

Vickram Srinivas et al. Cell Cycle. .

Abstract (VSports手机版)

Chondrocytes in the growth plate and articular cartilage and osteocytes subsumed in Haversian bone exist in environmental niches that are characterized by a limited oxygen supply. In these tissues, cells display a hitherto unrecognized state in which there is evidence of autophagy. The autophagic condition serves to promote cell survival. When the response is triggered, the cell cannibalizes itself to generate energy; if extended, then it can activate Type II apoptosis VSports手机版. We opine that survival is dependent on niche conditions and regulated by crosstalk between mTOR, AMPK and HIF-1 and HIF-2. Recent studies suggest that HIF-2 is a potent regulator of chondrocyte autophagy and that this protein acts as a brake to the stimulatory function of HIF-1. Accordingly, the oxemic state of the tissue, its nutrient supply as well as the energetic state of the cells regulates autophagic flux. From a clinical viewpoint, it may be possible to enhance skeletal cell survival through drugs that modulate the autophagic state and prevent the induction of apoptosis. .

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"V体育安卓版" Figures

Figure 1
Figure 1. Microenvironmental factors regulating autophagy on mineralizing cells
Under conditions of hypoxic stress, HIF-1 is stabilized leading to an energy charge dependent activation of AMPK. In addition, there is an increase in HIF-1 mediated REDD-1 expression. Thus, mTOR is inactivated resulting in a stimulation of autophagic flux. In parallel, an increase HIF-2 expression results in the dismutation of ROS, potent activators of autophagy. The reciprocal activities of HIF-1 and HIF-2 influence cell survival-death decisions.
See this image and copyright information in PMC

References

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    1. Terkhorn SP, Bohensky J, Shapiro IM, Koyama E, Srinivas V. Expression of HIF prolyl hydroxylase isozymes in growth plate chondrocytes: Relationship between maturation and apoptotic sensitivity. J Cell Physiol. 210:257–265. - PubMed
    1. Schipani E, Ryan HE, Didrickson S, Kobayashi T, Knight M, Johnson RS. Hypoxia in cartilage: HIF-1alpha is essential for chondrocyte growth arrest and survival. Genes Dev. 15:2865–2876. - "VSports注册入口" PMC - PubMed
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    1. Kronenberg HM. Developmental regulation of the growth plate. Nature. 423:332–336. - PubMed

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