ER stress

endoplasmic reticulum stress

ER stress unfolded protein response.

The unfolded protein response is mediated by several proteins that reside in and span the ER membrane. The luminal domains of these proteins sense perturbations in protein folding, and the cytoplasmic domains activate signaling pathways that reduce the levels of misfolded proteins in the cell, by increasing the production of chaperones and slowing down protein translation.

Paradoxically, the activation of the unfolded protein response also nduced by unfolded and misfolded proteins. Unfolded or misfolded proteins accumulate in the ER and trigger a number of cellular responses, collectively called the leads to cell death by activating caspases, particularly an ER-resident caspase called caspase-12 (CASP12).

Thus, misfolded proteins initially trigger the cytoprotective function of this response, but if these abnormal proteins persist, the pro-apoptotic cytotoxic functions take over. Aggregation of abnormally folded proteins, caused by genetic mutations, aging, or unknown environmental factors, is now recognized as a feature of a number of neurodegenerative diseases, including Alzheimer disease, Huntington disease, and Parkinson disease, and possibly type II diabetes.

Deprivation of glucose and oxygen, and stress such as heat, also result in protein misfolding and trigger the unfolded protein response, culminating in cell injury and death.

Pathology

endoplasmic reticulum stress

RNA translation diseases
- Wolcott-Rallison syndrome

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ER stress

endoplasmic reticulum stress

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