T Cell Immunity to Lymphoma Following Treatment with Anti-CD40 Monoclonal Antibody

Tutt, Alison L.; O’Brien, Lyn M.; Hussain, Akmal; Crowther, Graham; French, Ruth R.; Glennie, Martin J.

doi:10.4049/jimmunol.168.6.2720

Cited by 78 publications

(67 citation statements)

References 43 publications

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“…Interaction with its trimeric ligand on activated T cells results in APC activation, required for the induction of adaptive immunity (28,29). In preclinical models, rat anti-mouse CD40 mAb show remarkable therapeutic activity in the treatment of CD40 positive B cell lymphomas as well as various CD40-negative tumors (20,24,25). In our studies of therapeutic mAb, their potency is unprecedented, clearing bulk tumors from mice with established disease and providing immunity to rechallenge (20,24).…”

mentioning

confidence: 96%

“…Our work has focused on immunostimulatory anti-CD40 mAb (20,(23)(24)(25), which are also in clinical development (26,27). Reagents targeting this molecule have been investigated for .20 y and include both mAb and CD40L (20,26).…”

mentioning

confidence: 99%

“…In preclinical models, rat anti-mouse CD40 mAb show remarkable therapeutic activity in the treatment of CD40 positive B cell lymphomas as well as various CD40-negative tumors (20,24,25). In our studies of therapeutic mAb, their potency is unprecedented, clearing bulk tumors from mice with established disease and providing immunity to rechallenge (20,24). To date, four anti-CD40 mAb 893 (31), , HCD122 (26,33)], and Chi LOB7-4 (34) have been investigated in phase I/II trials.…”

mentioning

confidence: 99%

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Interaction with FcγRIIB Is Critical for the Agonistic Activity of Anti-CD40 Monoclonal Antibody

White

Chan

Roghanian

et al. 2011

The Journal of Immunology

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A high activatory/inhibitory FcγR binding ratio is critical for the activity of mAb such as rituximab and alemtuzumab that attack cancer cells directly and eliminate them by recruiting immune effectors. Optimal FcγR binding profiles of other anti-cancer mAb, such as immunostimulatory mAb that stimulate or block immune receptors, are less clear. In this study, we analyzed the importance of isotype and FcγR interactions in controlling the agonistic activity of the anti-mouse CD40 mAb 3/23. Mouse IgG1 (m1) and IgG2a (m2a) variants of the parental 3/23 (rat IgG2a) were engineered and used to promote humoral and cellular responses against OVA. The mouse IgG1 3/23 was highly agonistic and outperformed the parental Ab when promoting Ab (10–100-fold) and T cell (OTI and OTII) responses (2- to >10-fold). In contrast, m2a was almost completely inactive. Studies in FcγR knockout mice demonstrated a critical role for the inhibitory FcγRIIB in 3/23 activity, whereas activatory FcγR (FcγRI, -III, and -IV) was dispensable. In vitro experiments established that the stimulatory effect of FcγRIIB was mediated through Ab cross-linking delivered in trans between neighboring cells and did not require intracellular signaling. Intriguingly, activatory FcγR provided effective cross-linking of 3/23 m2a in vitro, suggesting the critical role of FcγRIIB in vivo reflects its cellular distribution and bioavailability as much as its affinity for a particular Ab isotype. In conclusion, we demonstrate an essential cross-linking role for the inhibitory FcγRIIB in anti-CD40 immunostimulatory activity and suggest that isotype will be an important issue when optimizing reagents for clinical use.

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confidence: 96%

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confidence: 99%

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confidence: 99%

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Interaction with FcγRIIB Is Critical for the Agonistic Activity of Anti-CD40 Monoclonal Antibody

White

Chan

Roghanian

et al. 2011

The Journal of Immunology

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197

219

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“…More importantly, the presence of these immunosuppressive factors might even result in alternative activated DCs that have acquired a strong T cell-tolerizing capacity after exposure to maturation stimuli. This could also explain the discrepancy between CD40 treatment of mice bearing s.c. tumors and AC tumors (26,34), as systemic anti-CD40 treatment in animals could perhaps not induce the desired maturation level of the eye-derived APC required for CTL induction, but rather an alternative activated DC endowed with the capacity to tolerize T cell responses. Because the unique microenvironment of the eye might prevent proper DC activation after CD40 ligation combined with the observation that AC tumor Ag can be presented to CTLs, it is tempting to speculate that neutralizing eye-derived APC-modulating cytokines will greatly improve immune intervention protocols.…”

Section: Discussionmentioning

confidence: 99%

“…It has been shown that anti-CD40 treatment can be a very powerful method to improve tumor-specific CTL immunity in tumorbearing mice, leading to the eradication of otherwise lethal tumors (26,34). CD40 signaling has been shown to be a very powerful way to enhance tumor-specific immunity, most likely through the activation of DCs (35,36) that cross-present tumor Ags to CTLs, as also exemplified by the up-regulation of activation markers and costimulatory molecules on CD11c ϩ cells after administration of anti-CD40 Abs (data not shown) (37).…”

Section: Systemic Cd40 Activation Does Not Lead To Eradication Of Thementioning

confidence: 99%

Intraocular Tumor Antigen Drains Specifically to Submandibular Lymph Nodes, Resulting in an Abortive Cytotoxic T Cell Reaction

Boonman

Mierlo

Fransen

et al. 2004

The Journal of Immunology

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Ocular immune privilege is considered essential in the protection against sight-threatening immune responses, as illustrated by the ability of the ocular environment to permit the growth of tumors that are rejected when implanted at other sites. Although several studies indicate that soluble Ag can drain directly into the spleen when injected into the anterior chamber, the primary site of intraocular tumor Ag presentation to tumor-specific CTLs has not been studied. To gain a better understanding of the mechanism involved in ocular immune privilege, we examined to which lymphoid organs anterior chamber tumor Ags primarily drain. Our data show that intraocular tumor Ag drains exclusively to the submandibular lymph nodes, resulting in activation of tumor-specific CTLs, whereas no Ag drainage was found in spleen. However, these tumor-specific CTLs do not distribute systemically and, as a consequence, intraocular tumor growth is unhampered. A similar lack of CTL efficacy has been observed in mice bearing s.c. tumors, which is converted to a systemic tumoricidal CTL response by administration of agonistic anti-CD40 mAb. In contrast, systemic anti-CD40 treatment of eye tumor-bearing mice did not result in mobilizing tumor-specific CTLs or tumor eradication. Together, these results show that intraocular tumor Ag drains to regional lymph nodes for activation of tumor-specific CTLs. However, the induced tumor-specific immunity is insufficient for tumor clearance, even combined with otherwise highly effective immune intervention protocols.

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Expression and costimulatory effects of the TNF receptor superfamily members CD134 (OX40) and CD137 (4-1BB), and their role in the generation of anti-tumor immune responses

et al. 2002

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This study addresses the relative importance of CD134 (OX40) and CD137 (4‐1BB) in the costimulation of CD4+ and CD8+ T cells under comparable conditions of antigenic stimulation. We demonstrate that CD134 is capable of directly costimulating CD8+ T cells. However, costimulation of CD8+ T cells by CD134 is less potent than that triggered by CD137. The higher costimulatory activity of CD137, when compared with CD134, correlates well with its faster expression kinetics and higher levels on CD8+ T cells. Furthermore, induction of CD137 expression on CD8+ T cells is highly sensitive to low levels of TCR stimulation, which is in contrast with CD134. Conversely, CD134 is more effective than CD137 in costimulating CD4+ T cells. This, however, could not be attributed to differential expression. We also demonstrate that the transient nature of CD134 and CD137 expression on activated CD4+ T cells is the resultof proteolytic shedding. Consistent with the greater ability of CD137 to costimulate CD8+ T cells, stimulation of CD137 in vivo is considerably more effective than CD134 in augmenting anti‐tumor immune responses. Therefore, agents that stimulate signaling via CD137 are likely to be more useful in clinical conditions where highly effective CD8+ CTL responses are required.

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T Cell Immunity to Lymphoma Following Treatment with Anti-CD40 Monoclonal Antibody

Cited by 78 publications

References 43 publications

Interaction with FcγRIIB Is Critical for the Agonistic Activity of Anti-CD40 Monoclonal Antibody

Interaction with FcγRIIB Is Critical for the Agonistic Activity of Anti-CD40 Monoclonal Antibody

Intraocular Tumor Antigen Drains Specifically to Submandibular Lymph Nodes, Resulting in an Abortive Cytotoxic T Cell Reaction

Expression and costimulatory effects of the TNF receptor superfamily members CD134 (OX40) and CD137 (4-1BB), and their role in the generation of anti-tumor immune responses

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