Rigosertib-Activated JNK1/2 Eliminate Tumor Cells through p66Shc Activation

Rigosertib-Activated JNK1/2 Eliminate Tumor Cells through p66Shc Activation

Rigosertib, via reactive oxygen species (ROS), stimulates cJun N-terminal kinases 1/2 (JNK1/2), which inactivate RAS/RAF signaling and thereby inhibit growth and survival of tumor cells. JNK1/2 are not only regulated by ROS-they in turn can also control ROS production. The prooxidant and cell death...

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Veröffentlicht in:Biology (Basel, Switzerland) Switzerland), 2020-05, Vol.9 (5), p.99
Hauptverfasser: Günther, Julia K, Nikolajevic, Aleksandar, Ebner, Susanne, Troppmair, Jakob, Khalid, Sana
Format: Artikel
Sprache:eng
Schlagworte:
Adapter proteins
Antibodies
Apoptosis
c-Jun N-terminal kinases
Cancer
Cell activation
Cell death
Control
DNA damage
Laboratories
Legal medicine
Oxidoreductase
p66Shc
Phosphorylation
Physiological aspects
Protein research
Raf protein
Reactive oxygen species
Rigosertib
Tumor cells
Tumors
Urology
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Zusammenfassung:Rigosertib, via reactive oxygen species (ROS), stimulates cJun N-terminal kinases 1/2 (JNK1/2), which inactivate RAS/RAF signaling and thereby inhibit growth and survival of tumor cells. JNK1/2 are not only regulated by ROS-they in turn can also control ROS production. The prooxidant and cell death function of p66Shc requires phosphorylation by JNK1/2. Here, we provide evidence that establishes p66Shc, an oxidoreductase, as a JNK1/2 effector downstream of Rigosertib-induced ROS production, DNA damage, and cell death. This may provide a common pathway for suppression of tumor cell growth by Rigosertib.
ISSN:2079-7737
2079-7737
DOI:10.3390/biology9050099