CD38‐Specific Gallium‐68 Labeled Peptide Radiotracer Enables Pharmacodynamic Monitoring in Multiple Myeloma with PET

Author:

Sharma Ajay Kumar1,Gupta Kuldeep1,Mishra Akhilesh12,Lofland Gabriela1,Marsh Ian3,Kumar Dhiraj1,Ghiaur Gabriel4,Imus Philip4,Rowe Steven P.1,Hobbs Robert F.3,Gocke Christian B.4,Nimmagadda Sridhar1456ORCID

Affiliation:

1. The Russell H. Morgan Department of Radiology and Radiological Science Johns Hopkins University School of Medicine Baltimore MD 21287 USA

2. Chemical & Biomolecular Engineering Whiting School of Engineering Johns Hopkins University Baltimore MD 21218 USA

3. Department of Radiation Oncology and Molecular Sciences Johns Hopkins University School of Medicine Baltimore MD 21287 USA

4. The Sidney Kimmel Comprehensive Cancer Center and the Bloomberg‐Kimmel Institute for Cancer Immunotherapy Johns Hopkins University School of Medicine Baltimore MD 21287 USA

5. Department of Pharmacology and Molecular Sciences Johns Hopkins University School of Medicine Baltimore MD 21287 USA

6. Division of Clinical Pharmacology Department of Medicine Johns Hopkins University School of Medicine Baltimore MD 21287 USA

Abstract

AbstractThe limited availability of molecularly targeted low‐molecular‐weight imaging agents for monitoring multiple myeloma (MM)‐targeted therapies has been a significant challenge in the field. In response, a first‐in‐class peptide‐based radiotracer, [68Ga]Ga‐AJ206, is developed that can be seamlessly integrated into the standard clinical workflow and is specifically designed to noninvasively quantify CD38 levels and pharmacodynamics by positron emission tomography (PET). A bicyclic peptide, AJ206, is synthesized and exhibits high affinity to CD38 (KD: 19.1 ± 0.99 × 10−9 m) by surface plasmon resonance. Further, [68Ga]Ga‐AJ206‐PET shows high contrast within 60 min and suitable absorbed dose estimates for clinical use. Additionally, [68Ga]Ga‐AJ206 detects CD38 expression in cell line‐derived xenografts, patient‐derived xenografts (PDXs), and disseminated disease models in a manner consistent with flow cytometry and immunohistochemistry findings. Moreover, [68Ga]Ga‐AJ206‐PET successfully quantifies CD38 pharmacodynamics in PDXs, revealing increased CD38 expression in the tumor following all‐trans retinoic acid (ATRA) therapy. In conclusion, [68Ga]Ga‐AJ206 exhibits the salient features required for clinical translation, providing CD38‐specific high‐contrast images in multiple models of MM. [68Ga]Ga‐AJ206‐PET could be useful for quantifying total CD38 levels and pharmacodynamics during therapy to evaluate approved and new therapies in MM and other diseases with CD38 involvement.

Funder

National Institutes of Health

Publisher

Wiley

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