Opportunistic Autoimmune Disorders Potentiated by Immune-Checkpoint Inhibitors Anti-CTLA-4 and Anti-PD-1

Kong, Yi; Flynn, Jeffrey C.

doi:10.3389/fimmu.2014.00206

Cited by 110 publications

(77 citation statements)

References 79 publications

(147 reference statements)

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“…Yet, the majority of cancer patients receiving immune-checkpoint blockade inhibitor therapy will develop autoimmune complications (15). In line with the findings reported in this article, these opportunistic autoimmune diseases seem to differ from classic organ-specific autoimmune diseases in their broader range of affected organs.…”

Section: Discussionsupporting

confidence: 81%

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The Contained Self-Reactive Peripheral T Cell Repertoire: Size, Diversity, and Cellular Composition

Richards

Ruggiero

Hofer

et al. 2015

The Journal of Immunology

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Individual self-reactive T cells have been discovered in both humans and mice. It is difficult to assess the entire contained self-reactive peripheral T cell repertoire in healthy individuals because regulatory T cells (Tregs) can render these cells anergic and, therefore, functionally indistinguishable. We addressed this issue by removing regulatory T cells, thereby allowing us to characterize the exposed self-reactive T cells. This resulted in activation of approximately 4% of both CD4+ and CD8+ T cells. Activation and division of these cells was not a bystander product of Ag-independent signals but required TCR stimulation. Analysis of TCR sequences showed that these responding cells were polyclonal and encompassed a broad range of structural TCR diversity. Adoptive transfer of naive and effector/memory T cell populations showed that even the naive T cell pool contained self-reactive T cell precursors. In addition, transfer of mature thymocytes showed that this response was an intrinsic T cell property rather than a peripheral adaptation. Finally, we found that the unexpectedly strong contribution of the naive CD5low T cell pool showed that the overall self-reactive response has not only a diverse polyclonal TCR repertoire, but also comprises a broad range of affinities for self.

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Section: Discussionsupporting

confidence: 81%

“…In fact, recent clinical trials with anti-CTLA-4 and anti-PD1 Abs uncovered that T cell reactivity against self is unleashed by these treatments. This now constitutes a major limitation for therapies that interfere with tolerance and immune homeostasis (15).…”

mentioning

confidence: 99%

The Contained Self-Reactive Peripheral T Cell Repertoire: Size, Diversity, and Cellular Composition

Richards

Ruggiero

Hofer

et al. 2015

The Journal of Immunology

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“…Additionally, recent studies demonstrate that immune checkpoint inhibitors can generate and/ or amplify an immune response against mutated antigens (37)(38)(39)(40). As a result of their systemic nature, these treatments can lead to severe autoimmune toxicities (41,42). The occurrence of severe autoimmune toxicities following treatment with an approach that targets neoantigens using MHC tetramer-sorted lymphocytes or cells engineered to express mutated epitope-specific TCRs is unlikely, however, as expression of these antigens is strictly limited to tumor cells.…”

Section: Discussionmentioning

confidence: 99%

Isolation of neoantigen-specific T cells from tumor and peripheral lymphocytes

Cohen

Gartner

Horovitz-Fried

et al. 2015

Journal of Clinical Investigation

335

275

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“…The frequency and type of irAE symptoms varied in clinical trials, depending on the nature of the target molecule and the patient cohort, the type and amount of Ab, as well as the particular protocol, and involved a range of tissues and organs. These symptoms led to dermatitis, enterocolitis, hepatitis, and wide spread endocrinopathies (hypophysitis, thyroiditis, adrenal insufficiency), with less frequent symptoms of uveitis, nephritis, arthritis, and inflammatory myopathy [6,34,35].…”

Section: Descriptionmentioning

confidence: 99%

Immune checkpoint-targeted therapy: cancer and autoimmune diseases represent two sides of the same coin

Isakov¹

2016

J Autoimmune Disord

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The immune system plays a critical role in tumor surveillance and cancer prevention. However, some cancer cells can evade immune destruction by acquiring the ability to inhibit immune checkpoint regulatory pathways and suppress anti-cancer immune responses. In recent years, the immune checkpoints took center stage in cancer immunotherapy and several promising strategies, based on the intervention in immune checkpointregulated pathways, have been designed in order to overcome mechanisms of immunosuppression. Clinical studies, using anti-inhibitory immune checkpoint-receptor antibodies, demonstrated durable clinical responses even in patients with advanced cancer. However, the clinical benefit was limited to a subset of cancer patients. Furthermore, the immune checkpoint therapy, which unleashes the immune system in order to augment the anti-cancer immune response, also increases the incidence of autoimmune diseases and induces an array of immune-related adverse effects. Here we briefly discuss some of the pros and cons of immune checkpoint-directed immunotherapy.

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Opportunistic Autoimmune Disorders Potentiated by Immune-Checkpoint Inhibitors Anti-CTLA-4 and Anti-PD-1

Cited by 110 publications

References 79 publications

The Contained Self-Reactive Peripheral T Cell Repertoire: Size, Diversity, and Cellular Composition

The Contained Self-Reactive Peripheral T Cell Repertoire: Size, Diversity, and Cellular Composition

Isolation of neoantigen-specific T cells from tumor and peripheral lymphocytes

Immune checkpoint-targeted therapy: cancer and autoimmune diseases represent two sides of the same coin

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