Is the “3+3” Dose-Escalation Phase I Clinical Trial Design Suitable for Therapeutic Cancer Vaccine Development? A Recommendation for Alternative Design

Rahma, Osama E.; Gammoh, Emily; Simon, Richard; Khleif, Samir N.

doi:10.1158/1078-0432.ccr-13-2671

Cited by 42 publications

(32 citation statements)

References 37 publications

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“…Imiquimod is not approved for use in topical treatment of melanoma metastases, but its off-label use has been reported in that setting (18, 28, 29), with beneficial control of treated lesions in some patients. Cancer vaccines have a very favorable safety profile (30) so the present study is consistent with prior work supporting safety of vaccines plus imiquimod in combination.…”

Section: Discussionsupporting

confidence: 89%

Topical treatment of melanoma metastases with imiquimod, plus administration of a cancer vaccine, promotes immune signatures in the metastases

Mauldin

Wages

Stowman

et al. 2016

Cancer Immunol Immunother

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Introduction Infiltration of cancers by T-cells is associated with improved patient survival and response to immune therapies; however, optimal approaches to induce T-cell infiltration of tumors are not known. This study was designed to assess whether topical treatment of melanoma metastases with the TLR7 agonist imiquimod plus administration of a multipeptide cancer vaccine will improve immune cell infiltration of melanoma metastases. Patients and Methods Eligible patients were immunized with a vaccine comprised of 12 melanoma peptides (12MP) and a tetanus toxoid-derived helper peptide, and imiquimod was applied topically to metastatic tumors daily. Adverse events were recorded and effects on the tumor microenvironment (TME) were evaluated from sequential tumor biopsies. T-cell responses were assessed by IFNγ ELIspot assay and T-cell tetramer staining. Patient tumors were evaluated for immune cell infiltration, cytokine and chemokine production, and gene expression. Results and Conclusions Four eligible patients were enrolled, and administration of imiquimod and vaccination were well-tolerated. Circulating T-cell responses to the vaccine were detected by ex vivo ELIspot assay in 3 of 4 patients. Treatment of metastases with imiquimod induced immune cell infiltration and favorable gene signatures in the patients with circulating T-cell responses. This study supports further study of topical imiquimod combined with vaccines or other immune therapies for the treatment of melanoma.

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Section: Discussionsupporting

confidence: 89%

Topical treatment of melanoma metastases with imiquimod, plus administration of a cancer vaccine, promotes immune signatures in the metastases

Mauldin

Wages

Stowman

et al. 2016

Cancer Immunol Immunother

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“…Most have a safety profile that is better than that of traditional cancer chemotherapies, with clinically significant adverse events being either not observed or only mild (18–20) (21). This of course is predicated on the ability to elicit a strong immune response in the setting of cancer.…”

Section: Review Of the Recommendations And Discussionmentioning

confidence: 99%

“…Accordingly, testing for acute toxicity in a phase 1 safety trial would be needed in the following categories: 1) any vaccine with substantial toxicity observed in preclinical toxicity studies; 2) classes of vaccine platforms with toxicity demonstrated in previously conducted clinical trials and 3) new vaccine platforms or other vaccine components (e.g. adjuvant) with potential vital organ toxicity (21). Since induction of autoimmunity is one of the safety issues that have been associated with some cancer vaccines, assessment of this issue in the earliest stage or NED patients with greater immune competence, is much more likely to be informative.…”

Section: Review Of the Recommendations And Discussionmentioning

confidence: 99%

“…Since phase 1 dose escalation studies of cancer vaccines do not determine toxicity or biologically active dose in the vast majority of the vaccines tested, another feasible goal of a phase 1 study in the premalignant setting, where individuals are expected to respond, could be to find a dose and a schedule that induces high levels of T helper 1 cell (TH1) and cytotoxic T lymphocytes (CTL) against tumor antigens while avoiding, to the extent possible, induction of immune suppressor cells (21). Therefore, in contrast to early phase trials with chemotherapy drugs, the most appropriate disease setting should involve patients who are not immunosuppressed and are capable of mounting a strong immune response to the vaccine.…”

Section: Review Of the Recommendations And Discussionmentioning

confidence: 99%

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The FDA Guidance on Therapeutic Cancer Vaccines: The Need for Revision to Include Preventive Cancer Vaccines or for a New Guidance Dedicated to Them

Finn

Khleif

Herberman³

2015

Cancer Prevention Research

Self Cite

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Cancer vaccines based on antigens derived from self molecules rather than pathogens, have been under basic and clinical investigations for many years. Up until very recently they had been tested primarily in the setting of metastatic disease with the goal to engage the immune system in slowing down disease progression. Many therapeutic vaccine trials, either investigator-initiated or led by pharmaceutical companies, have been completed and many are currently ongoing, following the FDA Guidance on therapeutic cancer vaccines published in 2011. In recent years the target of cancer vaccines is being shifted to early cancer and even premalignant disease with the goal of preventing cancer. While some issues addressed in the FDA Guidance on therapeutic vaccines apply to preventive vaccines, many do not. Here we discuss a set of recommendations for revising the current Guidance to also cover preventive vaccines, or to include in a new Guidance dedicated specifically to vaccines for cancer prevention.

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“…The Food and Drug Administration (FDA) recently published a “Guidance for Industry: Clinical Considerations for Therapeutic Cancer Vaccines,” which acknowledged the need for alternative dose-escalation methods in cancer vaccines [10, 11]. In contrast to chemotherapeutic agents, dose-finding in immunotherapy often investigates treatments that demonstrate minimal toxicity overall, where higher doses may not induce greater immunologic effect.…”

Section: Designing Immunotherapy Trialsmentioning

confidence: 99%

A Phase I/II adaptive design to determine the optimal treatment regimen from a set of combination immunotherapies in high-risk melanoma

Wages¹,

Slingluff²,

Petroni³

2015

Contemporary Clinical Trials

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In oncology, vaccine-based immunotherapy often investigates regimens that demonstrate minimal toxicity overall and higher doses may not correlate with greater immune response. Rather than determining the maximum tolerated dose, the goal of the study becomes locating the optimal biological dose, which is defined as a safe dose demonstrating the greatest immunogenicity, based on some predefined measure of immune response. Incorporation of adjuvants, new or optimized peptide vaccines, and combining vaccines with immune modulators may enhance immune response, with the aim of improving clinical response. Innovative dose escalation strategies are needed to establish the safety and immunogenicity of new immunologic combinations. We describe the implementation of an adaptive design for identifying the optimal treatment strategy in a multi-site, FDA-approved, phase I/II trial of a novel vaccination approach using long-peptides plus TLR agonists for resected stage IIB-IV melanoma. Operating characteristics of the design are demonstrated under various possible true scenarios via simulation studies. Overall performance indicates that the design is a practical Phase I/II adaptive method for use with combined immunotherapy agents. The simulation results demonstrate the method's ability to effectively recommend optimal regimens in a high percentage of trials with manageable sample sizes. The numerical results presented in this work include the type of simulation information that aid review boards in understanding design performance, such as average sample size and frequency of early trial termination, which we hope will augment early-phase trial design in cancer immunotherapy.

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Is the “3+3” Dose-Escalation Phase I Clinical Trial Design Suitable for Therapeutic Cancer Vaccine Development? A Recommendation for Alternative Design

Cited by 42 publications

References 37 publications

Topical treatment of melanoma metastases with imiquimod, plus administration of a cancer vaccine, promotes immune signatures in the metastases

Topical treatment of melanoma metastases with imiquimod, plus administration of a cancer vaccine, promotes immune signatures in the metastases

The FDA Guidance on Therapeutic Cancer Vaccines: The Need for Revision to Include Preventive Cancer Vaccines or for a New Guidance Dedicated to Them

A Phase I/II adaptive design to determine the optimal treatment regimen from a set of combination immunotherapies in high-risk melanoma

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