Uncoupling therapeutic from immunotherapy-related adverse effects for safer and effective anti-CTLA-4 antibodies in CTLA4 humanized mice

Du, Xuexiang; Liu, Mingyue; Su, Juanjuan; Zhang, Peng; Tang, Fei; Ye, Peiying; Devenport, Martin; Wang, Xu; Zhang, Yan; Liu, Yang

doi:10.1038/s41422-018-0012-z

Cited by 98 publications

(138 citation statements)

References 39 publications

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“…T-regs express high levels of CTLA4, and antibodies blocking CTLA4 can deplete T-regs in the TME in murine models, dependent on Fc subclass and host Fc receptor (42)(43)(44). T-reg depletion has also been hypothesized as a key mechanism of action for anti-CTLA4 treatment in humans (45,46), however clinical data does not support this (47), which may be due to the different isotype and Fc portion of the human antibody. Indeed, there is an association between pre-treatment Foxp3+ T-reg infiltration, followed by a subsequent increase in TILs 3 weeks into treatment in melanoma biopsies which was associated with response to the CTLA4-targeting antibody ipilimumab (48).…”

Section: T Cellsmentioning

confidence: 99%

Sensitizing the Tumor Microenvironment to Immune Checkpoint Therapy

et al. 2020

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Immune checkpoint blockade (ICB) has revolutionized cancer treatment, providing remarkable clinical responses in some patients. However, the majority of patients do not respond. It is therefore crucial both to identify predictive biomarkers of response and to increase the response rates to immune checkpoint therapy. In this review we explore the current literature about the predictive characteristics of the tumor microenvironment and discuss therapeutic approaches that aim to change this toward a milieu that is conducive to response. We propose a personalized biomarker-based adaptive approach to immunotherapy, whereby a sensitizing therapy is tailored to the patient's specific tumor microenvironment, followed by on-treatment verification of a change in the targeted biomarker, followed by immune checkpoint therapy. By incorporating detailed knowledge of the immunological tumor microenvironment, we may be able to sensitize currently non-responsive tumors to respond to immune checkpoint therapy.

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Section: T Cellsmentioning

confidence: 99%

Sensitizing the Tumor Microenvironment to Immune Checkpoint Therapy

et al. 2020

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“…29 In contrast, studies from several laboratories, including ours, established that selective depletion of regulatory T cells in the tumor microenvironment (TME) but not in the normal tissues as the primary mechanism of action of CITE. [29][30][31][32][33] The new understanding of regulatory T cell depletion explained why it is possible to uncouple irAE from CITE. 33,34 Unlike most cell-surface molecules, CTLA-4 recycles between the cell surface and endosomes, 35 where it is prevented from lysosomal degradation and recycles back to the cell surface by binding to the lipopolysaccharide-responsive and beige-like anchor (LRBA) protein.…”

Section: Introductionmentioning

confidence: 99%

“…[29][30][31][32][33] The new understanding of regulatory T cell depletion explained why it is possible to uncouple irAE from CITE. 33,34 Unlike most cell-surface molecules, CTLA-4 recycles between the cell surface and endosomes, 35 where it is prevented from lysosomal degradation and recycles back to the cell surface by binding to the lipopolysaccharide-responsive and beige-like anchor (LRBA) protein. 8,36 Since genetic mutations in either CTLA-4 5,8 or LRBA 8,36 cause autoimmune diseases in human, we hypothesize that anti-CTLA-4-induced irAE may relate to antibody-mediated disruption of CTLA-4 recycling.…”

Section: Introductionmentioning

confidence: 99%

Hijacking antibody-induced CTLA-4 lysosomal degradation for safer and more effective cancer immunotherapy

Zhang

Liu

et al. 2019

Cell Res

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It remains unclear why the clinically used anti-CTLA-4 antibodies, popularly called checkpoint inhibitors, have severe immunotherapy-related adverse effects (irAEs) and yet suboptimal cancer immunotherapeutic effects (CITE). Here we report that while irAE-prone Ipilimumab and TremeIgG1 rapidly direct cell surface CTLA-4 for lysosomal degradation, the non-irAE-prone antibodies we generated, HL12 or HL32, dissociate from CTLA-4 after endocytosis and allow CTLA-4 recycling to cell surface by the LRBA-dependent mechanism. Disrupting CTLA-4 recycling results in robust CTLA-4 downregulation by all anti-CTLA-4 antibodies and confers toxicity to a non-irAE-prone anti-CTLA-4 mAb. Conversely, increasing the pH sensitivity of TremeIgG1 by introducing designed tyrosine-to-histidine mutations prevents antibody-triggered lysosomal CTLA-4 downregulation and dramatically attenuates irAE. Surprisingly, by avoiding CTLA-4 downregulation and due to their increased bioavailability, pH-sensitive anti-CTLA-4 antibodies are more effective in intratumor regulatory T-cell depletion and rejection of large established tumors. Our data establish a new paradigm for cancer research that allows for abrogating irAE while increasing CITE of anti-CTLA-4 antibodies.

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“…Other groups have utilized human CTLA4 knockin models to interrogate irAE development in response to anti-CTLA4, anti-PD-1, or combination treatment (15). The examination of anti-CTLA4 DVD in the human CTLA4 mouse model would have strengthened the conclusions of Pai et al In addition, results from published studies regarding the effect of anti-CTLA4 therapy on Tregs in human tumors are varied, with some data suggesting these agents may not deplete Tregs (16), but may in fact expand the Treg pool (17) or even modulate Treg-suppressive function without actually affecting numbers (18).…”

Section: Limitations and Conclusionmentioning

confidence: 99%