Functional Differences between IgM and IgD Signaling in Chronic Lymphocytic Leukemia

Hacken, Elisa ten; Sivina, Mariela; Kim, Ekaterina; O’Brien, Susan; Wierda, William G.; Ferrajoli, Alessandra; Estrov, Zeev; Keating, Michael J.; Oellerich, Thomas; Scielzo, Cristina; Caligaris-Cappio, Federico; Burger, Jan A.

doi:10.4049/jimmunol.1600915

Cited by 35 publications

(29 citation statements)

References 56 publications

(70 reference statements)

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“…Most CLL cells express IgM receptors that, upon stimulation, activate signaling via the BCR, BTK, ERK, and AKT kinases to favor survival. 29 Our results demonstrating the ability of HDAC inhibitors singly or in combination with ibrutinib to effectively target BTK protein and abrogate its downstream signaling under conditions of IgM stimulation highlight the utility of this combination to antagonize the BCR-mediated survival advantage. In addition, because HDAC inhibitors can effectively also target mutated BTK in vitro, trials of HDAC inhibitors in treating ibrutinib-resistant CLL would be a rational strategy for patients with ibrutinib-resistant disease because survival for this group of patients is extremely poor.…”

Section: Discussionmentioning

confidence: 72%

“…Similar to cells exposed to abexinostat alone, there were time-dependent losses in p-PLCg2, p-ERK, and p-AKT, indicating the inhibition of BTK-mediated signaling ( Figure 5C). CLL cells respond to stimulation with IgM by activating BCR and BTK signaling to favor survival, 29 which was measured by increased p-ERK and p-AKT compared with their levels in unstimulated cells (supplemental Figure 5B). Exposure to ibrutinib inhibited p-BTK and For personal use only.…”

Section: Org Frommentioning

confidence: 99%

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Targeting BTK through microRNA in chronic lymphocytic leukemia

Bottoni

Rizzotto

Lai

et al. 2016

Blood

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Key Points• Inhibition of HDAC reverses epigenetic silencing to upregulate miRs that target BTK and suppress its downstream prosurvival signaling.• We identified a rationale for the dual targeting of BTK when combined with ibrutinib and a strategy to eliminate the C481S-mutant BTK clone.Bruton's tyrosine kinase (BTK) is a critical mediator of survival in B-cell neoplasms. Although BTK inhibitors have transformed therapy in chronic lymphocytic leukemia (CLL), patients with high-risk genetics are at risk for relapse and have a poor prognosis. Identification of novel therapeutic strategies for this group of patients is an urgent unmet clinical need, and therapies that target BTK via alternative mechanisms may fill this niche. Herein, we identify a set of microRNAs (miRs) that target BTK in primary CLL cells and show that the histone deacetylase (HDAC) repressor complex is recruited to these miR promoters to silence their expression. Targeting the HDACs by using either RNA interference against HDAC1 in CLL or a small molecule inhibitor (HDACi) in CLL and mantle cell lymphoma restored the expression of the BTK-targeting miRs with loss of BTK protein and downstream signaling and consequent cell death. We have also made the novel and clinically relevant discovery that inhibition of HDAC induces the BTK-targeting miRs in ibrutinib-sensitive and resistant CLL to effectively reduce both wild-type and C481S-mutant BTK. This finding identifies a novel strategy that may be promising as a therapeutic modality to eliminate the C481S-mutant BTK clone that drives resistance to ibrutinib and provides the rationale for a combination strategy that includes ibrutinib to dually target BTK to suppress its prosurvival signaling. (Blood. 2016;128(26):3101-3112)

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Section: Discussionmentioning

confidence: 72%

Section: Org Frommentioning

confidence: 99%

Targeting BTK through microRNA in chronic lymphocytic leukemia

Bottoni

Rizzotto

Lai

et al. 2016

Blood

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“…When the recently egressed and the persistently circulating fractions were identified by means of these markers, we observed that sIgM was higher in the recently egressed CLL cells. Interactions of CLL cells with tissue environmental cells will affect levels of functional BCR IgM/D complex (47). We and others have speculated that the higher sIgM might be a consequence of expression enhancement by tissue-derived IL4 (48,49).…”

Section: Discussionmentioning

confidence: 97%

Ibrutinib Therapy Releases Leukemic Surface IgM from Antigen Drive in Chronic Lymphocytic Leukemia Patients

Drennan

Chiodin

D’Avola

et al. 2019

Clinical Cancer Research

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Purpose: In chronic lymphocytic leukemia (CLL), disease progression associates with surface IgM (sIgM) levels and signaling capacity. These are variably downmodulated in vivo and recover in vitro, suggesting a reversible influence of tissuelocated antigen. Therapeutic targeting of sIgM function via ibrutinib, an inhibitor of Bruton tyrosine kinase (BTK), causes inhibition and tumor cell redistribution into the blood, with significant clinical benefit. Circulating CLL cells persist in an inhibited state, offering a tool to investigate the effects of drug on BTK-inhibited sIgM.Experimental Design: We investigated the consequences of ibrutinib therapy on levels and function of sIgM in circulating leukemic cells of patients with CLL.Results: At week 1, there was a significant increase of sIgM expression (64% increase from pretherapy) on CLL cells either recently released from tissue or persisting in blood. In contrast, surface IgD (sIgD) and a range of other receptors did not change. SIgM levels remained higher than pretherapy in the following 3 months despite gradual cell size reduction and ongoing autophagy and apoptotic activity. Conversely, IgD and other receptors did not increase and gradually declined. Recovered sIgM was fully N-glycosylated, another feature of escape from antigen, and expression did not increase further during culture in vitro. The sIgM was fully capable of mediating phosphorylation of SYK, which lies upstream of BTK in the Bcell receptor pathway.Conclusions: This specific IgM increase in patients underpins the key role of tissue-based engagement with antigen in CLL, confirms the inhibitory action of ibrutinib, and reveals dynamic adaptability of CLL cells to precision monotherapy. Figure 2.Surface expression of receptors on CLL cells during the first 3 months of ibrutinib therapy. PBMCs were taken at pre-, week 1, month 1, or month 3 of ibrutinib therapy and analyzed for cell surface marker expression taking into account CLL cell size. For each marker, the test MFI was divided by FSC 2 . Pretherapy values were normalized to one (white bar). Each bar represents mean with SEM. The statistical significance of difference was analyzed using the Wilcoxon signed rank test of the FSC-adjusted MFI values. Ã , P < 0.05; ÃÃ , P < 0.01; ÃÃÃ , P 0.001. Drennan et al.

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“…Interestingly, different BCR isotype stimulation played a role in B‐CLL. IgM signaling triggered B‐CLL cell survival via Erk activation, whereas IgD signaling induced phosphorylation of HS1 leading to BCR internalization and failure to induce B‐CLL cell survival . Thus, the type of BCR response may critically affect B‐CLL outcome which again involves HS1.…”

Section: Pathophysiologic Relevance Of Hs1mentioning

confidence: 99%

Hematopoietic cell-specific lyn substrate (HCLS1 or HS1): A versatile actin-binding protein in leukocytes

Castro-Ochoa

Guerrero‐Fonseca

Schnoor

2018

Journal of Leukocyte Biology

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Leukocytes are constantly produced in the bone marrow and released into the circulation. Many different leukocyte subpopulations exist that exert distinct functions. Leukocytes are recruited to sites of inflammation and combat the cause of inflammation via many different effector functions. Virtually all of these processes depend on dynamic actin remodeling allowing leukocytes to adhere, migrate, phagocytose, and release granules. However, actin dynamics are not possible without actin‐binding proteins (ABP) that orchestrate the balance between actin polymerization, branching, and depolymerization. The homologue of the ubiquitous ABP cortactin in hematopoietic cells is hematopoietic cell‐specific lyn substrate‐1, often called hematopoietic cell‐specific protein‐1 (HCLS1 or HS1). HS1 has been reported in different leukocytes to regulate Arp2/3‐dependent migration. However, more evidence is emerging that HS1 functions go far beyond just being a direct actin modulator. For example, HS1 is important for the activation of GTPases and integrins, and mediates signaling downstream of many receptors including BCR, TCR, and CXCR4. In this review, we summarize current knowledge on HS1 functions and discuss them in a pathophysiologic context.

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Functional Differences between IgM and IgD Signaling in Chronic Lymphocytic Leukemia

Cited by 35 publications

References 56 publications

Targeting BTK through microRNA in chronic lymphocytic leukemia

Targeting BTK through microRNA in chronic lymphocytic leukemia

Ibrutinib Therapy Releases Leukemic Surface IgM from Antigen Drive in Chronic Lymphocytic Leukemia Patients

Hematopoietic cell-specific lyn substrate (HCLS1 or HS1): A versatile actin-binding protein in leukocytes

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