Harnessing the Effects of BTKi on T Cells for Effective Immunotherapy against CLL

Mhibik, Maissa; Wiestner, Adrian; Sun, Clare

doi:10.3390/ijms21010068

Cited by 34 publications

(37 citation statements)

References 91 publications

(133 reference statements)

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“… 79 In addition, ibrutinib polarizes the T-cell population toward effector cells and reduces their exhaustion marker expression, which possibly enables the adaptive immune system to a more capable immune response. 56 , 80 B-cell activation and a subsequent increase in IgG levels, which are both inhibited by ibrutinib, are specifically increased in patients with severe COVID-19. 45 , 68 , 76 Because of these immunomodulatory effects, ibrutinib, and perhaps the more selective BTK inhibitors as well, might be beneficial in the early and late stages of COVID-19.…”

Section: Immunomodulation In Relation To Sars-cov-2mentioning

confidence: 99%

“… 54 Ibrutinib, as well as the more selective BTK inhibitors, reduces the (over)activated T-cell state of CLL patients, as measured by lower plasma cytokine levels and decreased exhaustion. 47 , 55 , 56 These observations are probably the indirect result of on-target (BTK) effects on leukemia cells, resulting in decreased suppressive interactions of the malignant B cells with T cells. 57 Sorafenib and sunitinib treatment also results in lower PD-1 expression on CD4 + and CD8 + T cells in vivo and in vitro, respectively.…”

Section: Impact Of the Main Tkis On The Immune Responsementioning

confidence: 99%

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Kinase inhibitors developed for treatment of hematologic malignancies: implications for immune modulation in COVID-19

Jacobs

Eldering²,

Kater

2021

Blood Advances

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Tyrosine kinase inhibitors (TKIs) are used to target dysregulated signaling pathways in virtually all hematologic malignancies. Many of the targeted signaling pathways are also essential in nonmalignant immune cells. The current coronavirus severe acute respiratory syndrome coronavirus 2 pandemic catalyzed clinical exploration of TKIs in the treatment of the various stages of COVID-19, which are characterized by distinct immune-related complications. Most of the reported effects of TKIs on immune regulation have been explored in vitro, with different class-specific drugs having nonoverlapping target affinities. Moreover, many of the reported in vivo effects are based on artificial animal models or on observations made in symptomatic patients with a hematologic malignancy who often already suffer from disturbed immune regulation. Based on in vitro and clinical observations, we attempt to decipher the impact of the main TKIs approved or in late-stage development for the treatment of hematological malignancies, including inhibitors of Bruton’s tyrosine kinase, spleen tyrosine kinase, BCR-Abl, phosphatidylinositol 3-kinase/ mammalian target of rapamycin, JAK/STAT, and FMS-like tyrosine kinase 3, to provide a rationale for how such inhibitors could modify clinical courses of diseases, such as COVID-19.

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Section: Immunomodulation In Relation To Sars-cov-2mentioning

confidence: 99%

Section: Impact Of the Main Tkis On The Immune Responsementioning

confidence: 99%

Kinase inhibitors developed for treatment of hematologic malignancies: implications for immune modulation in COVID-19

Jacobs

Eldering²,

Kater

2021

Blood Advances

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“…In chronic lymphocytic leukemia (CLL), it has been demonstrated that ibrutinib profoundly reshapes the T cell compartment, improving T cell function. Ibrutinib induces expansion of memory T cells, Th1 polarization, reduces the expression of inhibitory receptors (i.e., PD-1 and CTL-4), and improves immune synapse between T cells and CLL cells [ 103 , 104 ]. However, no data are available for FL in this regard.…”

Section: T Cells: Fundamental Actors In Fl Pathogenesis Modulated mentioning

confidence: 99%

Follicular Lymphoma Microenvironment: An Intricate Network Ready for Therapeutic Intervention

Dobaño-López

Araujo-Ayala

Serrat

et al. 2021

Cancers

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Follicular Lymphoma (FL), the most common indolent non-Hodgkin’s B cell lymphoma, is a paradigm of the immune microenvironment’s contribution to disease onset, progression, and heterogeneity. Over the last few years, state-of-the-art technologies, including whole-exome sequencing, single-cell RNA sequencing, and mass cytometry, have precisely dissected the specific cellular phenotypes present in the FL microenvironment network and their role in the disease. In this already complex picture, the presence of recurring mutations, including KMT2D, CREBBP, EZH2, and TNFRSF14, have a prominent contributory role, with some of them finely tuning this exquisite dependence of FL on its microenvironment. This precise characterization of the enemy (FL) and its allies (microenvironment) has paved the way for the development of novel therapies aimed at dismantling this contact network, weakening tumor cell support, and reactivating the host’s immune response against the tumor. In this review, we will describe the main microenvironment actors, together with the current and future therapeutic approaches targeting them.

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“…Indeed, and at variance from chemoimmunotherapy, ibrutinib mitigates the immune dysregulation induced by CLL, by modifying the absolute number of T-cells (25)(26)(27)(28), the T-cell receptor repertoire (26,29), the T-cell maturation (27,28), the Th1 and Th2 polarization (24)(25)(26)(27), the Th17 and Treg cell balance (25,27,28), the T cell inhibitory receptors and function (25,(27)(28)(29). These effects, all modulated toward an anti-tumor T-cell response, have been nicely reviewed (30)(31)(32). Regarding the Th1 and Th2 polarization, it has been shown that ibrutinib may contribute to revert the Th2-dominant response observed in CLL, thus influencing T-cell mediated cancer immune surveillance, in vitro and in a mouse model (24) and in patients treated with ibrutinib (25)(26)(27).…”

Section: Introductionmentioning

confidence: 99%

TH2/TH1 Shift Under Ibrutinib Treatment in Chronic Lymphocytic Leukemia

et al. 2021

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Ibrutinib may revert the T-helper (Th)2 polarization observed in chronic lymphocytic leukemia (CLL) by targeting the IL-2-inducible kinase, that shows a significant homology with the Bruton tyrosine kinase. In the front-line GIMEMA LLC1114 trial (ibrutinib+rituximab for 6 months, followed by ibrutinib maintenance), we investigated the modulation of T-cell cytokine production in 208 peripheral blood paired samples from 71 CLL patients: 71 samples prior to treatment (Day 0, D0) and at day +14 (D14; n=50), at month +8 (M8; 30), +12 (M12; 25), +18 (M18; 22) and +24 (M24; 10) of treatment. We documented a progressive decrease of CD3+CD4+IL-4+ T cells (Th2), that was significant at M8 and at M12 (p=0.019, p=0.002), a relative increase in the CD3+CD4+IFNγ+ T cells (Th1) and a decrease of CD3+CD4+IL-17+ (Th17) cells that was maintained up to M18 (M8 vs D0 p=0.003, M12 vs D0 p=0.003, M18 vs D0 p=0.004) of ibrutinib treatment. The Th2/Th1 ratio significantly decreased already after 14 days of treatment and was maintained thereafter (D14 vs D0 p=0.037, M8 vs D0 p=0.001, M12 vs D0 p=0.005, M18 vs D0 p=0.002). The Th2/Th1 modulation over time was significant only among patients with unmutated IGHV. The Th2/Th1 ratio below a cut-off of 0.088 at M8 was associated with the achievement of a complete response (CR) (p=0.016). Ibrutinib may shape the CLL T-cell profile, limiting Th2 activation and inducing a shift in the Th2/Th1 ratio. The association between the Th2/Th1 ratio decrease and the CR achievement suggests the in vivo generation of a potential host anti-tumor immune activation induced by ibrutinib.

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Harnessing the Effects of BTKi on T Cells for Effective Immunotherapy against CLL

Cited by 34 publications

References 91 publications

Kinase inhibitors developed for treatment of hematologic malignancies: implications for immune modulation in COVID-19

Kinase inhibitors developed for treatment of hematologic malignancies: implications for immune modulation in COVID-19

Follicular Lymphoma Microenvironment: An Intricate Network Ready for Therapeutic Intervention

TH2/TH1 Shift Under Ibrutinib Treatment in Chronic Lymphocytic Leukemia

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