Mixed-lineage kinase 3 phosphorylates prolyl-isomerase Pin1 to regulate its nuclear translocation and cellular function

Velusamy Rangasamy; Rajakishore Mishra; Gautam Sondarva; Subhasis Das; Tae Ho Lee; Joanna C. Bakowska; Guri Tzivion; James S. Malter; Basabi Rana; Kun Ping Lu; Anumantha Kanthasamy; Ajay Rana

doi:10.1073/pnas.1200804109

Mixed-lineage kinase 3 phosphorylates prolyl-isomerase Pin1 to regulate its nuclear translocation and cellular function

Velusamy Rangasamy, Rajakishore Mishra, Gautam Sondarva, Subhasis Das, Tae Ho Lee, Joanna C. Bakowska, Guri Tzivion, James S. Malter, Basabi Rana, Kun Ping Lu, Anumantha Kanthasamy, Ajay Rana

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Abstract

Nuclear protein peptidyl-prolyl isomerase Pin1-mediated prolyl isomerization is an essential and novel regulatory mechanism for protein phosphorylation. Therefore, tight regulation of Pin1 localization and catalytic activity is crucial for its normal nuclear functions. Pin1 is commonly dysregulated during oncogenesis and likely contributes to these pathologies; however, the mechanism( s) by which Pin1 catalytic activity and nuclear localization are increased is unknown. Here we demonstrate that mixed-lineage kinase 3 (MLK3), a MAP3K family member, phosphorylates Pin1 on a Ser138 site to increase its catalytic activity and nuclear translocation. This phosphorylation event drives the cell cycle and promotes cyclin D1 stability and centrosome amplification. Notably, Pin1 pSer138 is significantly up-regulated in breast tumors and is localized in the nucleus. These findings collectively suggest that the MLK3-Pin1 signaling cascade plays a critical role in regulating the cell cycle, centrosome numbers, and oncogenesis.

Original language	English (US)
Pages (from-to)	8149-8154
Number of pages	6
Journal	Proceedings of the National Academy of Sciences of the United States of America
Volume	109
Issue number	21
DOIs	https://doi.org/10.1073/pnas.1200804109
State	Published - May 22 2012

Keywords

Breast cancer
JNK

ASJC Scopus subject areas

General

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10.1073/pnas.1200804109

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Rangasamy, V., Mishra, R., Sondarva, G., Das, S., Lee, T. H., Bakowska, J. C., Tzivion, G., Malter, J. S., Rana, B., Lu, K. P., Kanthasamy, A., & Rana, A. (2012). Mixed-lineage kinase 3 phosphorylates prolyl-isomerase Pin1 to regulate its nuclear translocation and cellular function. Proceedings of the National Academy of Sciences of the United States of America, 109(21), 8149-8154. https://doi.org/10.1073/pnas.1200804109

Mixed-lineage kinase 3 phosphorylates prolyl-isomerase Pin1 to regulate its nuclear translocation and cellular function. / Rangasamy, Velusamy; Mishra, Rajakishore; Sondarva, Gautam et al.
In: Proceedings of the National Academy of Sciences of the United States of America, Vol. 109, No. 21, 22.05.2012, p. 8149-8154.

Research output: Contribution to journal › Article › peer-review

Rangasamy, V, Mishra, R, Sondarva, G, Das, S, Lee, TH, Bakowska, JC, Tzivion, G, Malter, JS, Rana, B, Lu, KP, Kanthasamy, A & Rana, A 2012, 'Mixed-lineage kinase 3 phosphorylates prolyl-isomerase Pin1 to regulate its nuclear translocation and cellular function', Proceedings of the National Academy of Sciences of the United States of America, vol. 109, no. 21, pp. 8149-8154. https://doi.org/10.1073/pnas.1200804109

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abstract = "Nuclear protein peptidyl-prolyl isomerase Pin1-mediated prolyl isomerization is an essential and novel regulatory mechanism for protein phosphorylation. Therefore, tight regulation of Pin1 localization and catalytic activity is crucial for its normal nuclear functions. Pin1 is commonly dysregulated during oncogenesis and likely contributes to these pathologies; however, the mechanism( s) by which Pin1 catalytic activity and nuclear localization are increased is unknown. Here we demonstrate that mixed-lineage kinase 3 (MLK3), a MAP3K family member, phosphorylates Pin1 on a Ser138 site to increase its catalytic activity and nuclear translocation. This phosphorylation event drives the cell cycle and promotes cyclin D1 stability and centrosome amplification. Notably, Pin1 pSer138 is significantly up-regulated in breast tumors and is localized in the nucleus. These findings collectively suggest that the MLK3-Pin1 signaling cascade plays a critical role in regulating the cell cycle, centrosome numbers, and oncogenesis.",

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author = "Velusamy Rangasamy and Rajakishore Mishra and Gautam Sondarva and Subhasis Das and Lee, {Tae Ho} and Bakowska, {Joanna C.} and Guri Tzivion and Malter, {James S.} and Basabi Rana and Lu, {Kun Ping} and Anumantha Kanthasamy and Ajay Rana",

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AU - Bakowska, Joanna C.

AU - Tzivion, Guri

AU - Malter, James S.

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AU - Lu, Kun Ping

AU - Kanthasamy, Anumantha

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AB - Nuclear protein peptidyl-prolyl isomerase Pin1-mediated prolyl isomerization is an essential and novel regulatory mechanism for protein phosphorylation. Therefore, tight regulation of Pin1 localization and catalytic activity is crucial for its normal nuclear functions. Pin1 is commonly dysregulated during oncogenesis and likely contributes to these pathologies; however, the mechanism( s) by which Pin1 catalytic activity and nuclear localization are increased is unknown. Here we demonstrate that mixed-lineage kinase 3 (MLK3), a MAP3K family member, phosphorylates Pin1 on a Ser138 site to increase its catalytic activity and nuclear translocation. This phosphorylation event drives the cell cycle and promotes cyclin D1 stability and centrosome amplification. Notably, Pin1 pSer138 is significantly up-regulated in breast tumors and is localized in the nucleus. These findings collectively suggest that the MLK3-Pin1 signaling cascade plays a critical role in regulating the cell cycle, centrosome numbers, and oncogenesis.

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Mixed-lineage kinase 3 phosphorylates prolyl-isomerase Pin1 to regulate its nuclear translocation and cellular function

Abstract

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