4/12/2023 0 Comments Kodi diagnozov po f 16chnStable E1A plus p53DD-transformed BMK cell lines were derived from the foci from bax −/−, bak −/−, and bax −/− bak −/− mice in the BMK cell transformation assay and were characterized for their ability to undergo apoptosis by death receptor signaling pathways. Thus, merely an increase in the amount of Bax or Bak may not result in cell death. Evidence suggests that Bax and Bak undergo changes in protein conformation that have been linked to their pro-apoptotic function (, ). ![]() Although there is up-regulation of bax, bak, puma, and noxa by p53, transcriptional up-regulation of at least Bax is not sufficient for p53-mediated apoptosis, because a mutant of p53 that up-regulates bax is not able to induce apoptosis. This caspase activation initiates a caspase cascade that is required for p53-dependent apoptosis (, ) and results in DNA fragmentation, cleavage of cellular proteins such as poly(ADP-ribose) polymerase and nuclear lamins, and cell death by apoptosis. In many cases, this event is pivotal in the regulation of apoptosis, because cytochrome c in the cytosol complexes with APAF-1 and, in turn, promotes caspase-9 activation. Cytochrome c release from the mitochondria occurs in many apoptotic signaling pathways including those implemented by p53 and TNF-α. ![]() ![]() ![]() Evidence suggests that Bax and Bak function is required for the release of cytochrome c from the mitochondria to the cytosol during apoptosis (, ).
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