<scp>CD</scp>27 costimulation contributes substantially to the expansion of functional memory <scp>CD</scp>8<sup>+</sup><scp>T</scp> cells after peptide immunization

Taraban, Vadim Y.; Rowley, Tania F.; Kerr, Jonathan P.; Willoughby, Jane E.; Johnson, Peter; Al‐Shamkhani, Aymen; Buchan, Sarah L.

doi:10.1002/eji.201343579

Cited by 31 publications

(30 citation statements)

References 56 publications

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“…CD27 stimulation significantly increases the magnitude of T cell responses to peptide or protein antigen in murine models [3••;17;60•] and synergizes with IFN-1 in both the expansion of effector CD8 + T cells and the subsequent development of CD8 + T cell memory. As the variegated influences of CD27 on effector and memory T cell development become more understood, there may be opportunities select regimens to support central, effector or tissue resident memory cells.…”

Section: Therapeutic Implementation Of Targeting Cd27mentioning

confidence: 99%

Stimulating CD27 to quantitatively and qualitatively shape adaptive immunity to cancer

Bullock

2017

Current Opinion in Immunology

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The capacity of the immune system to recognize and respond to tumors has been appreciated for over 100 years. However, clinical success has largely depended on the elucidation of the positive and negative regulators of effector cells after activation via the antigen cell receptor. On the one hand, effector cells upregulate checkpoint molecules that are thought to play a role in limiting immunopathology. On the other, second and third waves of costimulation are often required to promote the expansion, survival and differentiation of effector cells. While it is clear that the immune system can be unleashed by blocking checkpoint molecules, this approach is most effective when preexisting responses exist in patients. Thus, coordinating checkpoint blockade with costimulation could potentially expand the patient population that receives benefit from cancer immunotherapy. This review will discuss how the costimulatory molecule CD27 sculpts immunity and preclinical/clinical data indicating its potential for cancer immunotherapy and its clinical translation.

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Section: Therapeutic Implementation Of Targeting Cd27mentioning

confidence: 99%

Stimulating CD27 to quantitatively and qualitatively shape adaptive immunity to cancer

Bullock

2017

Current Opinion in Immunology

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“…These results stand in reasonably sharp contrast to the role of these receptors in a vaccine setting, where the blockade of CD27 produces dramatic (>10 fold) inhibition of the primary expansion of CD8 T cells [9–15, 45, 57–59]. Curiously, OX40 can serve as a reasonable substitute to support CD8+ T cell expansion to vaccination, but only in the developmental absence (KO animals) of CD27[12].…”

Section: T Cell Vs B Cell Fauna… All About the Numbersmentioning

confidence: 99%

“…OX40 has a less obscure role in CD4 cell response to vaccination where both CD27 and OX40 signaling are required for peak responses in the WT host [45]. While we have studied this extensively in response to the combined innate/CD40 vaccine adjuvant, others, using a diversity of immunization platforms (adjuvants, in vitro derived DCs, etc) have observed a similar importance for CD27 in a vaccine-elicited T cell response [9–15, 45, 57–59]. In the majority of these systems, this CD27 dependency influences expansion, survival and programming of effectors and memory.…”

Section: T Cell Vs B Cell Fauna… All About the Numbersmentioning

confidence: 99%

“…In contrast, IL-27 signaling appears to be required for the T cell responses to a host of subunit adjuvants [2], while the response to infectious challenge is either unaffected or even elevated in the absence of this cytokine [3, 4]. TNF receptor superfamily members expressed by T cells largely enhance various qualitative aspects of the T cell responses during infection [5–8], but instead dictate the quantitative magnitude of the response in subunit vaccine settings [9–15]. In short, the success or failure to produce a cellular response by subunit vaccination may be guided by different underlying mechanisms than those that govern infectious challenge.…”

Section: Introductionmentioning

confidence: 99%

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T Cell Vaccinology: Beyond the Reflection of Infectious Responses

Pennock

Kedl

2016

Trends in Immunology

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Inducing sustained, robust CD8+ T cell responses is necessary for therapeutic intervention in chronic infectious diseases and cancer. Unfortunately, most adjuvant formulations fail to induce substantial cellular immunity in humans. Attenuated acute infectious agents induce strong CD8+ T cell immunity, and are thought to therefore represent a good road map for guiding the development of subunit vaccines capable of inducing the same. However, recent evidence suggests that this assumption may need reconsideration. Here we provide an overview of subunit vaccine history as it pertains to instigating T cell responses. We argue that in light of evidence demonstrating that T cell responses to vaccination differ from those induced by infectious challenge, research in pursuit of cellular immunity-inducing vaccine adjuvants should no longer follow only the infection paradigm.

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“…CLL cells express both cell surface and soluble CD27 [20] and blocking the release of sCD27 using MMP-9 inhibitors induce higher levels of accessory molecules such as CD54, CD80 and CD95 [21]. Recent studies have confirmed functions for CD27 in T cell activation [22,23] and chronic myelogenous leukemia [24]; however, less data is available regarding CD27 function in normal B cells or CLL cells. One study using mouse models suggested a B cell intrinsic function of CD27 in germinal center responses [25].…”

Section: Introductionmentioning

confidence: 99%

Differential expression and function of CD27 in chronic lymphocytic leukemia cells expressing ZAP-70

et al. 2015

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CD27 costimulation contributes substantially to the expansion of functional memory CD8⁺T cells after peptide immunization

Cited by 31 publications

References 56 publications

Stimulating CD27 to quantitatively and qualitatively shape adaptive immunity to cancer

Stimulating CD27 to quantitatively and qualitatively shape adaptive immunity to cancer

T Cell Vaccinology: Beyond the Reflection of Infectious Responses

Differential expression and function of CD27 in chronic lymphocytic leukemia cells expressing ZAP-70

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CD27 costimulation contributes substantially to the expansion of functional memory CD8+T cells after peptide immunization

Cited by 31 publications

References 56 publications

Stimulating CD27 to quantitatively and qualitatively shape adaptive immunity to cancer

Stimulating CD27 to quantitatively and qualitatively shape adaptive immunity to cancer

T Cell Vaccinology: Beyond the Reflection of Infectious Responses

Differential expression and function of CD27 in chronic lymphocytic leukemia cells expressing ZAP-70

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CD27 costimulation contributes substantially to the expansion of functional memory CD8⁺T cells after peptide immunization