PKC-β as a therapeutic target in CLL: PKC inhibitor AEB071 demonstrates preclinical activity in CLL

El‐Gamal, Dalia; Williams, Katie; LaFollette, Taylor D.; Cannon, Matthew; Blachly, James S.; Zhong, Yun‐Shi; Woyach, Jennifer A.; Williams, Erich; Awan, Farrukh T.; Jones, Jeffrey; Andritsos, Leslie A.; Maddocks, Kami J.; Wu, Chia Hsien; Chen, Ching Shih; Lehman, Amy; Zhang, Xiaoli; Lapalombella, Rosa; Byrd, John C.

doi:10.1182/blood-2014-05-574830

Cited by 46 publications

(29 citation statements)

References 62 publications

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“…In multiple myeloma, pharmacologic inhibition of activated PKCbII using enzastaurin inhibited growth factors and cytokines secreted by multiple myeloma-derived bone marrow stromal cells (28). In CLL, PKCb is immediately downstream of the B-cell receptor and has been shown to be important to CLL cell autocrine survival and proliferation in vivo (43). PKCb is also essential for the development of CLL in the TCL1 transgenic mouse model, making it a valid therapeutic target in this malignancy (44).…”

Section: Discussionmentioning

confidence: 99%

MIF-Induced Stromal PKCβ/IL8 Is Essential in Human Acute Myeloid Leukemia

et al. 2017

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Acute myeloid leukemia (AML) cells exhibit a high level of spontaneous apoptosis when cultured in vitro but have a prolonged survival time in vivo, indicating that tissue microenvironment plays a critical role in promoting AML cell survival. In vitro studies have shown that bone marrow mesenchymal stromal cells (BM-MSC) protect AML blasts from spontaneous and chemotherapy-induced apoptosis. Here, we report a novel interaction between AML blasts and BM-MSCs, which benefits AML proliferation and survival. We initially examined the cytokine profile in cultured human AML compared with AML cultured with BM-MSCs and found that macrophage migration inhibitory factor (MIF) was highly expressed by primary AML, and that IL8 was increased in AML/BM-MSC cocultures. Recombinant MIF increased IL8 expression in BMMSCs via its receptor CD74. Moreover, the MIF inhibitor ISO-1 inhibited AML-induced IL8 expression by BM-MSCs as well as BM-MSC-induced AML survival. Protein kinase C b (PKCb) regulated MIF-induced IL8 in BM-MSCs. Finally, targeted IL8 shRNA inhibited BM-MSC-induced AML survival. These results describe a novel, bidirectional, prosurvival mechanism between AML blasts and BM-MSCs. Furthermore, they provide biologic rationale for therapeutic strategies in AML targeting the microenvironment, specifically MIF and IL8.

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Section: Discussionmentioning

confidence: 99%

MIF-Induced Stromal PKCβ/IL8 Is Essential in Human Acute Myeloid Leukemia

et al. 2017

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“…49 In support of this, AEB071 is currently being studied in a phase II clinical trial in diffuse large B-cell lymphoma, and has recently been demonstrated to have pre-clinical activity in CLL in vitro and in vivo. 50 Targeting PKC, and in particular PKCb, is especially pertinent given the recent findings of Lutzny et al, who demonstrated that PKCbII expression in bone marrow stromal cells is essential for the survival and development of CLL cells. 51 Therefore, inhibition of PKCb may modify the tumor microenvironment, which has been established to play a critical role in supporting CLL survival, proliferation and chemoresistance.…”

Section: Discussionmentioning

confidence: 99%

Generation of a poor prognostic chronic lymphocytic leukemia-like disease model: PKC subversion induces up-regulation of PKC II expression in B lymphocytes

et al. 2015

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“…For those with PCLG2 mutations or BTK mutations, other downstream targets such as PKCb might also be clinically relevant. Preclinical testing with sotrastaurin has shown proof of concept in this area 35 ; however, clinical studies are not being pursued in this population with this particular agent.…”

Section: Other Promising Drugs and Targetsmentioning

confidence: 99%

How I manage ibrutinib-refractory chronic lymphocytic leukemia

Woyach

2017

Blood

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The introduction of the Bruton tyrosine kinase (BTK) inhibitor ibrutinib has dramatically changed the management of chronic lymphocytic leukemia (CLL). Although responses have been durable in the majority of patients, relapses do occur, especially in the high-risk patient population. Most relapses occur as the result of acquired mutations in BTK and PLCG2, which may facilitate success with alternative targeted therapies. As outcomes after ibrutinib relapse have been reported to be poor, specific strategies are needed for this patient population. Here, I discuss the diagnosis and management of ibrutinib-refractory CLL. The focus will be on common clinical scenarios that can be mistaken for relapse and how to accurately determine which patients are relapsing. Because there is no established standard of care, I discuss currently available options for standard therapy and existing clinical data. I also discuss new agents with the potential to be effective in patients refractory to ibrutinib. Finally, I discuss strategies for long-term disease control in this patient population.

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PKC-β as a therapeutic target in CLL: PKC inhibitor AEB071 demonstrates preclinical activity in CLL

Cited by 46 publications

References 62 publications

MIF-Induced Stromal PKCβ/IL8 Is Essential in Human Acute Myeloid Leukemia

MIF-Induced Stromal PKCβ/IL8 Is Essential in Human Acute Myeloid Leukemia

Generation of a poor prognostic chronic lymphocytic leukemia-like disease model: PKC subversion induces up-regulation of PKC II expression in B lymphocytes

How I manage ibrutinib-refractory chronic lymphocytic leukemia

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