CDK4 Expression and Activity Are Required for Cytokine Responsiveness in T Cells

Modiano, Jaime F.; Mayor, Jocelyne; Ball, Carrie R.; Fuentes, Maryse; Linthicum, D. Scott

doi:10.4049/jimmunol.165.12.6693

Cited by 29 publications

(37 citation statements)

References 59 publications

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“…Preclinical studies showed that CDK4/6 inhibitor pretreatment protects both cancer cells and normal hematopoietic cells from death induced by ionizing radiation and other DNA-damaging agents (38). Similarly, antigen-stimulated T cells are dependent on CDK4/6 activity for proliferative expansion and differentiation (39), suggesting that combinations of CDK4/6 inhibitors with immune checkpoint inhibitors (e.g., anti-PD-1) will require careful evaluation for potential antagonism in preclinical models and human subjects.…”

Section: Therapeutic Applications Of Cdk4/6 Inhibitorsmentioning

confidence: 99%

Molecular Pathways: Targeting the Cyclin D–CDK4/6 Axis for Cancer Treatment

VanArsdale

Boshoff

Arndt

et al. 2015

Clinical Cancer Research

324

240

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Cancer cells bypass normal controls over mitotic cell-cycle progression to achieve a deregulated state of proliferation. The retinoblastoma tumor suppressor protein (pRb) governs a key cell-cycle checkpoint that normally prevents G 1 -phase cells from entering S-phase in the absence of appropriate mitogenic signals. Cancer cells frequently overcome pRbdependent growth suppression via constitutive phosphorylation and inactivation of pRb function by cyclin-dependent kinase (CDK) 4 or CDK6 partnered with D-type cyclins.

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Section: Therapeutic Applications Of Cdk4/6 Inhibitorsmentioning

confidence: 99%

Molecular Pathways: Targeting the Cyclin D–CDK4/6 Axis for Cancer Treatment

VanArsdale

Boshoff

Arndt

et al. 2015

Clinical Cancer Research

324

240

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“…It is known that these proteins contribute to the regulation of normal lymphocyte proliferation, possibly providing mechanisms that enforce quiescence, 15 but their precise role in the pathogenesis of NHL remains incompletely understood. In human NHL, alterations leading to p16 inactivation (deletion or promoter methylation) are commonly seen in blastoid mantle cell lymphoma; they occur less frequently in association with progression from mucosal associated lymphoid tissue lymphoma or follicular lymphoma to diffuse large B-cell lymphoma (DLBCL), and only sporadically in high-grade tumors.…”

mentioning

confidence: 99%

Predictive value of p16 or Rb inactivation in a model of naturally occurring canine non-Hodgkin's lymphoma

et al. 2006

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“…Moreover, Cdk4 is clearly required for cytokine responsiveness in T cells (47). Surface markers on the lymphocyte and myeloid compartments in the prediabetic period reveal that both male and female NOD/Cdk4R24C cells present a more activated phenotype than WT gender-matched cells.…”

Section: Discussionmentioning

confidence: 99%

Cyclin-Dependent Kinase 4 Hyperactivity Promotes Autoreactivity in the Immune System but Protects Pancreatic β Cell Mass from Autoimmune Destruction in the Nonobese Diabetic Mouse Model

Marzo

Ortega²,

Stratmann

et al. 2008

The Journal of Immunology

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Cyclin-dependent kinase 4 (Cdk4) plays a central role in perinatal pancreatic β cell replication, thus becoming a potential target for therapeutics in autoimmune diabetes. Its hyperactive form, Cdk4R24C, causes β cell hyperplasia without promoting hypoglycemia in a nonautoimmune-prone mouse strain. In this study, we explore whether β cell hyperproliferation induced by the Cdk4R24C mutation balances the autoimmune attack against β cells inherent to the NOD genetic background. To this end, we backcrossed the Cdk4R24C knockin mice, which have the Cdk4 gene replaced by the Cdk4R24C mutated form, onto the NOD genetic background. In this study, we show that NOD/Cdk4R24C knockin mice exhibit exacerbated diabetes and insulitis, and that this exacerbated diabetic phenotype is solely due to the hyperactivity of the NOD/Cdk4R24C immune repertoire. Thus, NOD/Cdk4R24C splenocytes confer exacerbated diabetes when adoptively transferred into NOD/SCID recipients, compared with NOD/wild-type (WT) donor splenocytes. Accordingly, NOD/Cdk4R24C splenocytes show increased basal proliferation and higher activation markers expression compared with NOD/WT splenocytes. However, to eliminate the effect of the Cdk4R24C mutation specifically in the lymphocyte compartment, we introduced this mutation into NOD/SCID mice. NOD/SCID/Cdk4R24C knockin mice develop β cell hyperplasia spontaneously. Furthermore, NOD/SCID/Cdk4R24C knockin females that have been adoptively transferred with NOD/WT splenocytes are more resistant to autoimmunity than NOD/SCID WT female. Thus, the Cdk4R24C mutation opens two avenues in the NOD model: when expressed specifically in β cells, it provides a new potential strategy for β cell regeneration in autoimmune diabetes, but its expression in the immune repertoire exacerbates autoimmunity.

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CDK4 Expression and Activity Are Required for Cytokine Responsiveness in T Cells

Cited by 29 publications

References 59 publications

Molecular Pathways: Targeting the Cyclin D–CDK4/6 Axis for Cancer Treatment

Molecular Pathways: Targeting the Cyclin D–CDK4/6 Axis for Cancer Treatment

Predictive value of p16 or Rb inactivation in a model of naturally occurring canine non-Hodgkin's lymphoma

Cyclin-Dependent Kinase 4 Hyperactivity Promotes Autoreactivity in the Immune System but Protects Pancreatic β Cell Mass from Autoimmune Destruction in the Nonobese Diabetic Mouse Model

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