PIM1 kinase promotes gallbladder cancer cell proliferation via inhibition of proline-rich Akt substrate of 40 kDa (PRAS40)

Tejaswini Subbannayya; Pamela Leal-Rojas; Alex Zhavoronkov; Ivan V. Ozerov; Mikhail Korzinkin; Niraj Babu; Aneesha Radhakrishnan; Sandip Chavan; Remya Raja; Sneha M. Pinto; Arun H. Patil; Mustafa A. Barbhuiya; Prashant Kumar; Rafael Guerrero-Preston; Sanjay Navani; Pramod K. Tiwari; Rekha Vijay Kumar; T. S.Keshava Prasad; Juan Carlos Roa; Akhilesh Pandey; David Sidransky; Harsha Gowda; Evgeny Izumchenko; Aditi Chatterjee

doi:10.1007/s12079-018-00503-5

PIM1 kinase promotes gallbladder cancer cell proliferation via inhibition of proline-rich Akt substrate of 40 kDa (PRAS40)

Tejaswini Subbannayya, Pamela Leal-Rojas, Alex Zhavoronkov, Ivan V. Ozerov, Mikhail Korzinkin, Niraj Babu, Aneesha Radhakrishnan, Sandip Chavan, Remya Raja, Sneha M. Pinto, Arun H. Patil, Mustafa A. Barbhuiya, Prashant Kumar, Rafael Guerrero-Preston, Sanjay Navani, Pramod K. Tiwari, Rekha Vijay Kumar, T. S.Keshava Prasad, Juan Carlos Roa, Akhilesh PandeyDavid Sidransky, Harsha Gowda, Evgeny Izumchenko, Aditi Chatterjee

Laboratory Medicine and Pathology

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

5 Scopus citations

Abstract

Gallbladder cancer (GBC) is a rare malignancy, associated with poor disease prognosis with a 5-year survival of only 20%. This has been attributed to late presentation of the disease, lack of early diagnostic markers and limited efficacy of therapeutic interventions. Elucidation of molecular events in GBC can contribute to better management of the disease by aiding in the identification of therapeutic targets. To identify aberrantly activated signaling events in GBC, tandem mass tag-based quantitative phosphoproteomic analysis of five GBC cell lines was carried out. Proline-rich Akt substrate 40 kDa (PRAS40) was one of the proteins found to be hyperphosphorylated in all the invasive GBC cell lines. Tissue microarray-based immunohistochemical labeling of phospho-PRAS40 (T246) revealed moderate to strong staining in 77% of the primary gallbladder adenocarcinoma cases. Regulation of PRAS40 activity by inhibiting its upstream kinase PIM1 resulted in a significant decrease in cell proliferation, colony forming and invasive ability of GBC cells. Our results support the role of PRAS40 phosphorylation in GBC cell survival and aggressiveness. This study also elucidates phospho-PRAS40 as a clinical marker in GBC and the role of PIM1 as a therapeutic target in GBC.

Original language	English (US)
Pages (from-to)	163-177
Number of pages	15
Journal	Journal of Cell Communication and Signaling
Volume	13
Issue number	2
DOIs	https://doi.org/10.1007/s12079-018-00503-5
State	Published - Jun 6 2019

Keywords

Cell survival
Gastrointestinal cancer
Phosphoproteomics
SGI-1776
Targeted therapy
mTOR signaling

ASJC Scopus subject areas

Biochemistry
Molecular Biology
Cell Biology

Access to Document

10.1007/s12079-018-00503-5

Cite this

Subbannayya, T., Leal-Rojas, P., Zhavoronkov, A., Ozerov, I. V., Korzinkin, M., Babu, N., Radhakrishnan, A., Chavan, S., Raja, R., Pinto, S. M., Patil, A. H., Barbhuiya, M. A., Kumar, P., Guerrero-Preston, R., Navani, S., Tiwari, P. K., Kumar, R. V., Prasad, T. S. K., Roa, J. C., ... Chatterjee, A. (2019). PIM1 kinase promotes gallbladder cancer cell proliferation via inhibition of proline-rich Akt substrate of 40 kDa (PRAS40). Journal of Cell Communication and Signaling, 13(2), 163-177. https://doi.org/10.1007/s12079-018-00503-5

Subbannayya, T, Leal-Rojas, P, Zhavoronkov, A, Ozerov, IV, Korzinkin, M, Babu, N, Radhakrishnan, A, Chavan, S, Raja, R, Pinto, SM, Patil, AH, Barbhuiya, MA, Kumar, P, Guerrero-Preston, R, Navani, S, Tiwari, PK, Kumar, RV, Prasad, TSK, Roa, JC, Pandey, A, Sidransky, D, Gowda, H, Izumchenko, E & Chatterjee, A 2019, 'PIM1 kinase promotes gallbladder cancer cell proliferation via inhibition of proline-rich Akt substrate of 40 kDa (PRAS40)', Journal of Cell Communication and Signaling, vol. 13, no. 2, pp. 163-177. https://doi.org/10.1007/s12079-018-00503-5

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title = "PIM1 kinase promotes gallbladder cancer cell proliferation via inhibition of proline-rich Akt substrate of 40 kDa (PRAS40)",

abstract = "Gallbladder cancer (GBC) is a rare malignancy, associated with poor disease prognosis with a 5-year survival of only 20%. This has been attributed to late presentation of the disease, lack of early diagnostic markers and limited efficacy of therapeutic interventions. Elucidation of molecular events in GBC can contribute to better management of the disease by aiding in the identification of therapeutic targets. To identify aberrantly activated signaling events in GBC, tandem mass tag-based quantitative phosphoproteomic analysis of five GBC cell lines was carried out. Proline-rich Akt substrate 40 kDa (PRAS40) was one of the proteins found to be hyperphosphorylated in all the invasive GBC cell lines. Tissue microarray-based immunohistochemical labeling of phospho-PRAS40 (T246) revealed moderate to strong staining in 77% of the primary gallbladder adenocarcinoma cases. Regulation of PRAS40 activity by inhibiting its upstream kinase PIM1 resulted in a significant decrease in cell proliferation, colony forming and invasive ability of GBC cells. Our results support the role of PRAS40 phosphorylation in GBC cell survival and aggressiveness. This study also elucidates phospho-PRAS40 as a clinical marker in GBC and the role of PIM1 as a therapeutic target in GBC.",

keywords = "Cell survival, Gastrointestinal cancer, Phosphoproteomics, SGI-1776, Targeted therapy, mTOR signaling",

author = "Tejaswini Subbannayya and Pamela Leal-Rojas and Alex Zhavoronkov and Ozerov, {Ivan V.} and Mikhail Korzinkin and Niraj Babu and Aneesha Radhakrishnan and Sandip Chavan and Remya Raja and Pinto, {Sneha M.} and Patil, {Arun H.} and Barbhuiya, {Mustafa A.} and Prashant Kumar and Rafael Guerrero-Preston and Sanjay Navani and Tiwari, {Pramod K.} and Kumar, {Rekha Vijay} and Prasad, {T. S.Keshava} and Roa, {Juan Carlos} and Akhilesh Pandey and David Sidransky and Harsha Gowda and Evgeny Izumchenko and Aditi Chatterjee",

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doi = "10.1007/s12079-018-00503-5",

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T1 - PIM1 kinase promotes gallbladder cancer cell proliferation via inhibition of proline-rich Akt substrate of 40 kDa (PRAS40)

AU - Subbannayya, Tejaswini

AU - Leal-Rojas, Pamela

AU - Zhavoronkov, Alex

AU - Ozerov, Ivan V.

AU - Korzinkin, Mikhail

AU - Babu, Niraj

AU - Radhakrishnan, Aneesha

AU - Chavan, Sandip

AU - Raja, Remya

AU - Pinto, Sneha M.

AU - Patil, Arun H.

AU - Barbhuiya, Mustafa A.

AU - Kumar, Prashant

AU - Guerrero-Preston, Rafael

AU - Navani, Sanjay

AU - Tiwari, Pramod K.

AU - Kumar, Rekha Vijay

AU - Prasad, T. S.Keshava

AU - Roa, Juan Carlos

AU - Pandey, Akhilesh

AU - Sidransky, David

AU - Gowda, Harsha

AU - Izumchenko, Evgeny

AU - Chatterjee, Aditi

PY - 2019/6/6

Y1 - 2019/6/6

N2 - Gallbladder cancer (GBC) is a rare malignancy, associated with poor disease prognosis with a 5-year survival of only 20%. This has been attributed to late presentation of the disease, lack of early diagnostic markers and limited efficacy of therapeutic interventions. Elucidation of molecular events in GBC can contribute to better management of the disease by aiding in the identification of therapeutic targets. To identify aberrantly activated signaling events in GBC, tandem mass tag-based quantitative phosphoproteomic analysis of five GBC cell lines was carried out. Proline-rich Akt substrate 40 kDa (PRAS40) was one of the proteins found to be hyperphosphorylated in all the invasive GBC cell lines. Tissue microarray-based immunohistochemical labeling of phospho-PRAS40 (T246) revealed moderate to strong staining in 77% of the primary gallbladder adenocarcinoma cases. Regulation of PRAS40 activity by inhibiting its upstream kinase PIM1 resulted in a significant decrease in cell proliferation, colony forming and invasive ability of GBC cells. Our results support the role of PRAS40 phosphorylation in GBC cell survival and aggressiveness. This study also elucidates phospho-PRAS40 as a clinical marker in GBC and the role of PIM1 as a therapeutic target in GBC.

AB - Gallbladder cancer (GBC) is a rare malignancy, associated with poor disease prognosis with a 5-year survival of only 20%. This has been attributed to late presentation of the disease, lack of early diagnostic markers and limited efficacy of therapeutic interventions. Elucidation of molecular events in GBC can contribute to better management of the disease by aiding in the identification of therapeutic targets. To identify aberrantly activated signaling events in GBC, tandem mass tag-based quantitative phosphoproteomic analysis of five GBC cell lines was carried out. Proline-rich Akt substrate 40 kDa (PRAS40) was one of the proteins found to be hyperphosphorylated in all the invasive GBC cell lines. Tissue microarray-based immunohistochemical labeling of phospho-PRAS40 (T246) revealed moderate to strong staining in 77% of the primary gallbladder adenocarcinoma cases. Regulation of PRAS40 activity by inhibiting its upstream kinase PIM1 resulted in a significant decrease in cell proliferation, colony forming and invasive ability of GBC cells. Our results support the role of PRAS40 phosphorylation in GBC cell survival and aggressiveness. This study also elucidates phospho-PRAS40 as a clinical marker in GBC and the role of PIM1 as a therapeutic target in GBC.

KW - Cell survival

KW - Gastrointestinal cancer

KW - Phosphoproteomics

KW - SGI-1776

KW - Targeted therapy

KW - mTOR signaling

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