A Novel Requirement for Janus Kinases as Mediators of Drug Resistance Induced by Fibroblast Growth Factor-2 in Human Cancer Cells

A Mantovani; A Verma; AF Wilks; Ana P. Costa-Pereira; AP Costa-Pereira; C Schindler; Catarina R. Carmo; CV Ramana; D Hanahan; D Watling; DE Levy; E Chen; G Packham; H Yu; I Sakai; IM Kerr; J Ragimbeau; Janet Lyons-Lewis; JS Bezbradica; KM Kozopas; L Song; M Karaghiosoff; M Pesu; Michael J. Seckl; O Simma; OE Pardo; OE Pardo; OE Pardo; OE Pardo; OE Pardo; P Krejci; P Salven; R Beroukhim; Rakesh K. Srivastava; S Radtke; S Song; T Ben-Zvi; T Ruotsalainen; U Graeven; X Yang; Y Qing

A Novel Requirement for Janus Kinases as Mediators of Drug Resistance Induced by Fibroblast Growth Factor-2 in Human Cancer Cells

Authors: A Mantovani
A Verma
AF Wilks
Ana P. Costa-Pereira
AP Costa-Pereira
C Schindler
Catarina R. Carmo
CV Ramana
D Hanahan
D Watling
DE Levy
E Chen
G Packham
H Yu
I Sakai
IM Kerr
J Ragimbeau
Janet Lyons-Lewis
JS Bezbradica
KM Kozopas
L Song
M Karaghiosoff
M Pesu
Michael J. Seckl
O Simma
OE Pardo
OE Pardo
OE Pardo
OE Pardo
OE Pardo
P Krejci
P Salven
R Beroukhim
Rakesh K. Srivastava
S Radtke
S Song
T Ben-Zvi
T Ruotsalainen
U Graeven
X Yang
Y Qing
Publication date: 5 April 2011
Publisher: Public Library of Science
Doi

Abstract

The development of resistance to chemotherapy is a major cause of cancer-related death. Elucidating the mechanisms of drug resistance should thus lead to novel therapeutic strategies. Fibroblast growth factor (FGF)-2 signaling induces the assembly of a multi-protein complex that provides tumor cells with the molecular machinery necessary for drug resistance. This complex, which involves protein kinase C (PKC) ε, v-raf murine sarcoma viral oncogene homolog B1 (B-RAF) and p70 S6 kinase β (S6K2), enhances the selective translation of anti-apoptotic proteins such as B-cell leukaemia/lymphoma-2 (BCL-2) and inhibitors of apoptosis protein (IAP) family members and these are able to protect multiple cancer cell types from chemotherapy-induced cell death. The Janus kinases (JAKs) are most noted for their critical roles in mediating cytokine signaling and immune responses. Here, we show that JAKs have novel functions that support their consideration as new targets in therapies aimed at reducing drug resistance. As an example, we show that the Janus kinase TYK2 is phosphorylated downstream of FGF-2 signaling and required for the full phosphorylation of extracellular signal-regulated kinase (ERK) 1/2. Moreover, TYK2 is necessary for the induction of key anti-apoptotic proteins, such as BCL-2 and myeloid cell leukemia sequence (MCL) 1, and for the promotion of cell survival upon FGF-2. Silencing JAK1, JAK2 or TYK2 using RNA interference (RNAi) inhibits FGF2-mediated proliferation and results in the sensitization of tumor cells to chemotherapy-induced killing. These effects are independent of activation of signal transducer and activator of transcription (STAT) 1, STAT3 and STAT5A/B, the normal targets of JAK signaling. Instead, TYK2 associates with the other kinases previously implicated in FGF-2-mediated drug resistance. In light of these findings we hypothesize that TYK2 and other JAKs are important modulators of FGF-2-driven cell survival and that inhibitors of these kinases will likely improve the effectiveness of other cancer therapies