2020
DOI: 10.18632/oncotarget.27508
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Roscovitine enhances all-trans retinoic acid (ATRA)-induced nuclear enrichment of an ensemble of activated signaling molecules and augments ATRA-induced myeloid cell differentiation

Abstract: Although ATRA represents a successful differentiation therapy for APL, it is largely ineffective for non-APL AMLs. Hence combination therapies using an agent targeting ATRA-regulated molecules that drive cell differentiation/arrest are of interest. Using the HL-60 human non-APL AML model where ATRA causes nuclear enrichment of c-Raf that drives differentiation/G0-arrest, we now observe that roscovitine enhanced nuclear enrichment of certain traditionally cytoplasmic signaling molecules and enhanced differentia… Show more

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Cited by 13 publications
(18 citation statements)
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References 66 publications
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“…Arguably the prototype is Raf. RA-induced signalsome activation is associated with nuclear enrichment of Raf [ 17 , 20 ]. The nuclear Raf binds the NFATc3 transcription factor on the promoter of CXCR5 downstream of a non-canonical RARE [ 16 ].…”
Section: Discussionmentioning
confidence: 99%
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“…Arguably the prototype is Raf. RA-induced signalsome activation is associated with nuclear enrichment of Raf [ 17 , 20 ]. The nuclear Raf binds the NFATc3 transcription factor on the promoter of CXCR5 downstream of a non-canonical RARE [ 16 ].…”
Section: Discussionmentioning
confidence: 99%
“…The proposed paradigm also offers a rationalization for why very diverse agents have been serendipitously found to enhance RA action. For example, arsenic trioxide (a poison that generates oxidative stress with widespread toxicological effects) [ 68 ], Bosutinib (originally introduced as an SFK inhibitor) [ 69 ], Roscovitine (originally introduced as a CDK inhibitor) [ 20 , 45 ], and RRD-251 (originally introduced as a small molecule targeting Raf interactions) [ 19 ] all enhance the effects of RA. These agents have in common that they also have unanticipated abilities to target and stimulate signalsome components.…”
Section: Discussionmentioning
confidence: 99%
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“…c-Raf phosphorylates transcription factors required for ATRA-induced differentiation [9]. Recently, Rashid et al [10, 11] used the t(15;17)-negative HL-60 human myeloblastic leukemia model and found that a CDK inhibitor, roscovitine, enhanced differentiation. Roscovitine also enhanced the ATRA-induced nuclear enrichment of several signaling molecules, including pS259- pS289/296/301- pS621-c-Raf, pS217/221-Mek, Src family kinases (SFKs), Lyn Fgr, adaptor proteins c-Cbl and SLP-76, guanine exchange factor Vav1, and transcription factor IRF-1, which are known to play important roles in not only proliferation but also differentiation [10].…”
Section: Cdk Inhibitorsmentioning
confidence: 99%
“…Roscovitine also enhanced the ATRA-induced nuclear enrichment of several signaling molecules, including pS259- pS289/296/301- pS621-c-Raf, pS217/221-Mek, Src family kinases (SFKs), Lyn Fgr, adaptor proteins c-Cbl and SLP-76, guanine exchange factor Vav1, and transcription factor IRF-1, which are known to play important roles in not only proliferation but also differentiation [10]. They further revealed that c-Raf or Lyn formed a complex with retinoblastoma (RB), and that the c-Raf- or Lyn-retinoblastoma association was greatly diminished by ATRA and lost in ATRA and roscovitine co-treated cells [11]. Furthermore, Lyn knockdown enhanced ATRA-induced differentiation markers, such as CD11b, G1/G0 arrest, and ROS production [10].…”
Section: Cdk Inhibitorsmentioning
confidence: 99%