A novel chemical strategy to harness the tumor specific biochemistry of human kallikrein 2 for prostate cancer theranostics
About This Grant
The recent FDA approvals (Lutathera, Azedra, Pluvicto) and the swell of promising experimental agents in clinical trials underscore the surging enthusiasm to investigate molecularly targeted radiotherapy (TRT) as a treatment modality for many cancers. However, the clinical experience shows that tumor responses to TRTs are often transient and/or variable among patients. Thus, there is an urgent unmet need to develop new strategies to maximize the therapeutic benefit of TRT for cancer patients. We have approached this challenge by developing a new class of radiopharmaceuticals termed “restricted interaction peptides” (RIPs) which are low molecular weight (MW) peptides that are internally cleaved by a tumor endoprotease to unmask a radiolabeled membrane binding peptide. After RIP proteolysis, the membrane binding peptide adopts a helical conformation and immediately attaches to a nearby plasma membranes in the tumor. Using PET, we have found that RIPs may have several properties advantageous for TRT. we hypothesize that RIPs may be a mutually safe and effective platform for TRT. During this project, we will test this hypothesis over three Specific Aims. During Aim 1, we will perform antitumor assessment studies with a radiolabeled RIP targeting human kallikrein 2 (hK2). We are prioritizing hK2 as the kallikreins are selectively produced by prostate cancer cells in patients with metastatic castration resistant prostate cancer (mCPRC), it is a highly efficient serine protease, and it is more highly and broadly expressed than PSMA. A promising lead (termed KRIP2.1) has been developed, validated as an hK2 substrate, radiolabeled with Cu-64, and confirmed via PET to target prostate cancer xenografts with no off target activation. During Aim 1, DOTA-KRIP2.1 will be conjugated to a representative β- (Lu-177) or alpha (Ac-225) emitter and its antitumor effects will be studied in mice bearing various tumor types with endogenous hK2 expression. During Aim 2, we will ask whether patient imaging with 64Cu-KRIP2.1 is feasible. A first in human study will be performed in 6 subjects (3 male, 3 female) to assess the safety, dosimetry, and pharmacokinetics of 64Cu-KRIP2.1. During Aim 3, we will ask whether tumor imaging with 64Cu-KRIP2.1 is feasible. Two cohorts representing patients with castration sensitive prostate cancer (n = 20) or mCRPC patients (n = 20) will receive 64Cu-KRIP2.1 PET/CT and the rate of detection will be benchmarked against anatomical imaging and immunohistochemical analysis for hK2 expression in biopsies. This project represents the first use of a conditionally activated membrane binding probe for TRT, which may overcome the well documented and significant shortcomings of conventional RLT. We are optimistic the data from these studies will provide a compelling rationale to initiate a drug trial for radiolabeled KRIP2.1 as well as to expand this platform to treat tumors overexpressing other extracellular endoproteases.
Grant Summary
A novel chemical strategy to harness the tumor specific biochemistry of human kallikrein 2 for prostate cancer theranostics is a NCI - National Cancer Institute grant providing up to $575K for university, nonprofit, healthcare org. Applications are due 2031-04-30 (open). Check eligibility and apply with FindGrants.
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Up to $575K
2031-04-30
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A novel chemical strategy to harness the tumor specific biochemistry of human kallikrein 2 for prostate cancer theranostics: Frequently Asked Questions
Who is eligible for the A novel chemical strategy to harness the tumor specific biochemistry of human kallikrein 2 for prostate cancer theranostics?
A novel chemical strategy to harness the tumor specific biochemistry of human kallikrein 2 for prostate cancer theranostics is offered by NCI - National Cancer Institute and is generally open to university, nonprofit, healthcare org. It is open to organizations nationwide unless the funder specifies otherwise. Review the specific eligibility terms before applying, since funders set their own requirements around organization type, location, and the population or project being served.
How much funding does the A novel chemical strategy to harness the tumor specific biochemistry of human kallikrein 2 for prostate cancer theranostics provide?
A novel chemical strategy to harness the tumor specific biochemistry of human kallikrein 2 for prostate cancer theranostics provides up to $575K per award from NCI - National Cancer Institute. Actual award sizes depend on the scope of your project, available program funds, and the number of applicants, so build a budget that reflects realistic, allowable costs rather than the maximum figure.
When is the A novel chemical strategy to harness the tumor specific biochemistry of human kallikrein 2 for prostate cancer theranostics deadline?
Applications for A novel chemical strategy to harness the tumor specific biochemistry of human kallikrein 2 for prostate cancer theranostics are due 2031-04-30 (open). Because deadlines can change, verify the date with the funder, NCI - National Cancer Institute, and give yourself enough time to prepare a complete, competitive application before the close date.
How do you apply for the A novel chemical strategy to harness the tumor specific biochemistry of human kallikrein 2 for prostate cancer theranostics?
To apply for A novel chemical strategy to harness the tumor specific biochemistry of human kallikrein 2 for prostate cancer theranostics, confirm your eligibility, gather the required documents, and prepare a narrative and budget that address the funder's priorities. FindGrants guides you step by step and can draft each section, then exports a submission-ready application pack for this grant from NCI - National Cancer Institute.