Inhibition of the growth of WI-38 fibroblasts by benzyloxycarbonyl-Leu-Leu-Tyr diazomethyl ketone: evidence that cleavage of p53 by a calpain-like protease is necessary for G1 to S-phase transition

Zhang, Wenli; Lü, Qing; Xie, Zijian; Mellgren, Ronald L.

doi:10.1038/sj.onc.1200841

Cited by 69 publications

(65 citation statements)

References 19 publications

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“…Induction of wild type p53 in MCF7 is a positive control for PS-341 activity resistant to ALLN (Figures 2a and 3c). Accumulation of wild type p53, previously shown to be sensitive to calpain as well as proteasome inhibition (Gonen et al, 1997;Kubbutat and Vousden, 1997;Pariat et al, 1997;Zhang et al, 1997), was demonstrated in MCF10 cells at the concentrations/incubation times used of the calpain inhibitors calpastatin peptide and PD150606 (Figure 4b). …”

Section: Brca1 Protein Accumulated After Alln Has An Increased Half-lifementioning

confidence: 77%

Regulation of BRCA1 by protein degradation

et al. 1999

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BRCA1, a tumor suppressor protein implicated in hereditary forms of breast and ovarian cancer, is transcriptionally regulated in a proliferation-dependent manner. In this study, we demonstrate a substantial role for proteolysis in regulating the BRCA1 steady-state protein level in several cell lines. N-acetyl-leu-leunorleucinal (ALLN), an inhibitor of the proteasome, calpain, and cathepsins, caused BRCA1 protein to accumulate in the nucleus of several human breast, prostate, and melanoma cell lines which express low or undetectable basal levels of BRCA1 protein, but not in cells with high basal expression of BRCA1. Protease inhibition did not increase BRCA1 synthesis, nor change its mRNA level, but it dramatically prolonged the protein's half-life. In contrast to ALLN, lactacystin and PS341, two speci®c proteasome inhibitors, as well as calpastatin peptide and PD150606, two selective calpain inhibitors, had no e ect on BRCA1 stability, whereas ALLM, an e ective calpain and cathepsin inhibitor but weak proteasome inhibitor, did stimulate accumulation of BRCA1. Moreover, three inhibitors of acidic cysteine proteases, chloroquine, ammonium chloride and ba®lo-mycin, were as e ective as ALLN. These results demonstrate that degradation by a cathepsin-like protease in ®ne balance with BRCA1 transcription is responsible for maintaining the low steady-state level of BRCA1 protein seen in many cancer cells.

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Section: Brca1 Protein Accumulated After Alln Has An Increased Half-lifementioning

confidence: 77%

Regulation of BRCA1 by protein degradation

et al. 1999

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“…Involvement of a calpain-like activity in G 1 3 S transitions has been suggested in other systems on the basis of indirect evidence (14,15). An S-phase delay has also been observed in P. berghei parasites lacking 1 of 2 eEF1a genes, but in that case, the total cell cycle was prolonged (16).…”

Section: Discussionmentioning

confidence: 96%

A calpain unique to alveolates is essential in Plasmodium falciparum and its knockdown reveals an involvement in pre-S-phase development

Russo

Oksman

Vaupel

et al. 2009

Proc. Natl. Acad. Sci. U.S.A.

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Plasmodium falciparum encodes a single calpain that has a distinct domain composition restricted to alveolates. To evaluate the potential of this protein as a drug target, we assessed its essentiality. Both gene disruption by double cross-over and gene truncation by single cross-over recombination failed. We were also unable to achieve allelic replacement by using a missense mutation at the catalytic cysteine codon, although we could obtain synonymous allelic replacement parasites. These results suggested that the calpain gene and its proteolytic activity are important for optimal parasite growth. To gain further insight into its biological role, we used the FKBP degradation domain system to generate a fusion protein whose stability in transfected parasites could be modulated by a small FKBP ligand, Shield1 (Shld1). We made a calpain-GFP-FKBP fusion through single cross-over integration at the endogenous calpain locus. Calpain levels were knocked down and parasite growth was greatly impaired in the absence of Shld1. Parasites were delayed in their ability to transition out of the ring stage and in their ability to progress to the S phase. Calpain is required for cell cycle progression in Plasmodium parasites and appears to be an attractive drug target. We have shown that regulated knockdowns are possible in P. falciparum and can be useful for evaluating essentiality and function.cell cycle ͉ cysteine protease ͉ essentiality ͉ inducible ͉ malaria

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“…Interference with the p53-JNK association reduced p53 ubiquitination and increased p53 half-life, suggesting that JNK might target p53 to ubiquitination and degradation (Fuchs et al, 1998). In addition to degradation by the proteasome, p53 has been shown to be cleaved by another protease, calpain, which may also serve to regulate p53 Pariat et al, 1997;Zhang et al, 1997;Atencio et al, 2000).…”

Section: Mdm2-independent Regulation Of P53 Stabilitymentioning

confidence: 99%

Activation and activities of the p53 tumour suppressor protein

Bálint¹,

Vousden²

2001

Br J Cancer

272

178

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The p53 tumour suppressor protein inhibits malignant progression by mediating cell cycle arrest, apoptosis or repair following cellular stress. One of the major regulators of p53 function is the MDM2 protein, and multiple forms of cellular stress activate p53 by inhibiting the MDM2-mediated degradation of p53. Mutations in p53, or disruption of the pathways that allow activation of p53, seem to be a general feature of all cancers. Here we review recent advances in our understanding of the pathways that regulate p53 and the pathways that are induced by p53, as well as their implications for cancer therapy. © 2001 Cancer Research Campaign http://www.bjcancer.com

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Inhibition of the growth of WI-38 fibroblasts by benzyloxycarbonyl-Leu-Leu-Tyr diazomethyl ketone: evidence that cleavage of p53 by a calpain-like protease is necessary for G1 to S-phase transition

Cited by 69 publications

References 19 publications

Regulation of BRCA1 by protein degradation

Regulation of BRCA1 by protein degradation

A calpain unique to alveolates is essential in Plasmodium falciparum and its knockdown reveals an involvement in pre-S-phase development

Activation and activities of the p53 tumour suppressor protein

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