2003
DOI: 10.1016/s1074-5521(02)00310-1
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Pin1 and Par14 Peptidyl Prolyl Isomerase Inhibitors Block Cell Proliferation

Abstract: Disruption of the parvulin family peptidyl prolyl isomerase (PPIase) Pin1 gene delays reentry into the cell cycle when quiescent primary mouse embryo fibroblasts are stimulated with serum. Since Pin1 regulates cell cycle progression, a Pin1 inhibitor would be expected to block cell proliferation. To identify such inhibitors, we screened a chemical compound library for molecules that inhibited human Pin1 PPIase activity in vitro. We found a set of compounds that inhibited Pin1 PPIase activity in vitro with low … Show more

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Cited by 163 publications
(163 citation statements)
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“…Although the deletion of Pin1 is not universally lethal (mice, D. melanogaster, and S. pombe), there is evidence suggesting that other isomerases can substitute for Pin1 in its absence. Drugs targeting the catalytic activity of both Pin1 and a parvulin family member, par14, have been demonstrated to block proliferation of numerous mammalian cell lines (56). Also, in S. pombe the disruption of Pin1 sensitizes the yeast to the cyclophilin inhibitor, cyclosporin A (6,57).…”
Section: Fig 5 Nima and Pina Physically Interactmentioning
confidence: 99%
“…Although the deletion of Pin1 is not universally lethal (mice, D. melanogaster, and S. pombe), there is evidence suggesting that other isomerases can substitute for Pin1 in its absence. Drugs targeting the catalytic activity of both Pin1 and a parvulin family member, par14, have been demonstrated to block proliferation of numerous mammalian cell lines (56). Also, in S. pombe the disruption of Pin1 sensitizes the yeast to the cyclophilin inhibitor, cyclosporin A (6,57).…”
Section: Fig 5 Nima and Pina Physically Interactmentioning
confidence: 99%
“…As functional compensation for Ess1/ Pin1 by cyclophilins A was observed in yeasts Huang et al, 2001), and the most differentially up-regulated gene/protein in Pin1 −/− MEFs was Par14, the second human parvulin representative turned out to be a likely candidate for overcoming the loss of Pin1. This idea was supported by the fact that siRNA depletion of Par14 inhibits the growth of Pin1 −/− MEF and inhibitors designed for acting on both parvulins increase the amount of S-phase cells in synchronized cell lines (Uchida et al, 2003). Moreover, Pin1 and Par14 have been found to be active in similar cellular events and pathways as summarized in Table 3.…”
Section: Is There a Cross-talk Between Human Parvulins?mentioning
confidence: 91%
“…Specific inhibitors for Par14 are missing. To our knowledge only the cell-permeable tetra-oxobenzo-phenanthroline inhibitors designed by Uchida and coworkers (Uchida et al, 2003) efficiently block PPIase activity of Pin1 as well as Par14 with comparable IC 50 values of ~1 μm in a PPIase assay. (Hennig et al, 1998) Pepti-cinnamine analogue 1 (PA1) 0.6 In cells Attacks and adds covalently to cysteine and /or lysine side chains;…”
Section: Inhibitorsmentioning
confidence: 96%
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