Rpn2, or Regulatory Particle Non-ATPase 2, is a critical component of the 19S regulatory particle, which is integral to the 26S proteasome complex. The 26S proteasome is a pivotal cellular machinery responsible for the selective degradation of ubiquitinated proteins. Through its degradation function, it maintains protein homeostasis, regulates various cellular processes, and manages the timely removal of misfolded or damaged proteins. Rpn2 specifically plays a role in the recognition and processing of proteins tagged for degradation by ubiquitin, which is a small protein that marks other proteins for proteolysis. By binding to ubiquitin chains, Rpn2 facilitates the transfer of target proteins to the proteolytic core of the proteasome. This activity is essential for the regulated turnover of proteins and for cellular responses to environmental and metabolic changes, ensuring cellular integrity and function.
The expression of Rpn2 may be influenced by a variety of chemical compounds, which are known to affect cellular pathways indirectly related to proteasome function. Compounds such as MG-132 and Bortezomib, both proteasome inhibitors, could stimulate the cellular compensatory mechanisms, leading to an upregulation of Rpn2 expression in an effort to restore homeostasis. Similarly, chemicals that induce cellular stress, such as Tunicamycin and Thapsigargin, which interfere with protein glycosylation and calcium homeostasis respectively, may also lead to an increase in Rpn2 levels as part of the unfolded protein response. Other stress-inducing agents like cadmium chloride and arsenic trioxide promote oxidative stress and could conceivably heighten Rpn2 expression as the cell seeks to cope with the ensuing protein damage. It is the intricate balance between protein synthesis, folding, and degradation that these diverse compounds tap into, potentially influencing the expression of key proteasomal components like Rpn2 in order to maintain cellular proteostasis.
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