Abstract

The objective of this basic/discovery research project is to develop combination therapies that enhance the efficacy of multiple myeloma (MM) killing by the nanotherapeutics being developed in Projects 1 and 2. Since experimental evidence continues to support a critical role for the BM microenvironment in mediating de novo drug resistance and disease progression in MM, targeted modulation of microenvironmental regulatory pathways may be essential to control MM. We plan to use preclinical mouse (5TGM1 cells in C57BL/KaLwRij mice) and human xenotransplant (MM.1S cells in NSG mice) models to test if modulation of the BM microenvironment improves the efficacy of the Project 1 and 2 nanotherapeutics via the following two aims:
Aim 1 : Test if BM niche disrupting agents enhance the efficacy of MM killing by the nanoparticles generated in Projects 1 and 2. We will determine if CXCR4 (G- CSF, AMD3100, ALT1188 & CMD peptide), VLA-4 (firategrast & firategrast analogues) and proteasome (bortezomib, carfilzomib, and ixazomib) inhibitors mobilize MM cells and increase nanoparticle-mediated MM killing.
Aim 2 : Test if anti-CD47 monoclonal antibodies (CD47mAbs) enhance the efficacy of MM killing by the nanoparticles generated in Projects 1 and 2. Leukemic cells increase CD47 expression to avoid phagocytic clearance. CD47mAbs that block the CD47/SIRP? interaction enhance phagocytosis of leukemia cells. We have identified two CD47mAbs, Vx-1000 and Vx-1004, both of which block the CD47/SIRP? interaction and promote phagocytosis of tumor cells by macrophages. However, Vx-1004 also has the unique property of killing cancer cells, but not normal blood cells, via a direct, cell- autonomous, cytotoxic mechanism. We will determine if the tumor-toxic activity of Vx- 1004 confers enhanced efficacy in vivo compared to Vx-1000 in promoting MM killing by the Project 1 and 2 nanotherapeutics. If the BM niche disrupting agents and/or CD47mAbs being examined in these preclinical studies enhance the efficacy of nanoparticle-mediated MM killing, we may have a novel therapeutic approach for sensitization of drug (including nanoparticle) resistant MM cells and for prevention of minimal residual disease in MM. Furthermore, these therapeutic approaches may pave the way for development of similar treatments for other hematologic and solid tumor malignancies.

Public Health Relevance

The bone marrow microenvironment plays a critical role in mediating drug resistance and disease progression in multiple myeloma. Targeted nanoparticles are emerging as promising agents for cancer therapy. In this project we are testing if disruption of the bone marrow microenvironment with novel anti-CD47 monoclonal antibodies and CXCR4, VLA-4 and proteasome inhibitors can enhance the killing of multiple myeloma cells by targeted nanoparticles.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Specialized Center--Cooperative Agreements (U54)
Project #
5U54CA199092-05
Application #
9747817
Study Section
Special Emphasis Panel (ZCA1)
Project Start
Project End
Budget Start
2019-08-01
Budget End
2020-07-31
Support Year
5
Fiscal Year
2019
Total Cost
Indirect Cost

  Institution

Name
Washington University
Department
Type
DUNS #
068552207
City
Saint Louis
State
MO
Country
United States
Zip Code
63130

  Publications

Ye, Dezhuang; Zhang, Xiaohui; Yue, Yimei et al. (2018) Focused ultrasound combined with microbubble-mediated intranasal delivery of gold nanoclusters to the brain. J Control Release 286:145-153
Miller, Jessica; Wang, Steven T; Orukari, Inema et al. (2018) Perfusion-based fluorescence imaging method delineates diverse organs and identifies multifocal tumors using generic near-infrared molecular probes. J Biophotonics 11:e201700232
Ye, Dezhuang; Sultan, Deborah; Zhang, Xiaohui et al. (2018) Focused ultrasound-enabled delivery of radiolabeled nanoclusters to the pons. J Control Release 283:143-150
Karakocak, Bedia Begum; Liang, Jue; Biswas, Pratim et al. (2018) Hyaluronate coating enhances the delivery and biocompatibility of gold nanoparticles. Carbohydr Polym 186:243-251
de la Puente, Pilar; Luderer, Micah J; Federico, Cinzia et al. (2018) Enhancing proteasome-inhibitory activity and specificity of bortezomib by CD38 targeted nanoparticles in multiple myeloma. J Control Release 270:158-176
White, Brian S; Lanc, Irena; O'Neal, Julie et al. (2018) A multiple myeloma-specific capture sequencing platform discovers novel translocations and frequent, risk-associated point mutations in IGLL5. Blood Cancer J 8:35
Cui, Grace; Akers, Walter J; Scott, Michael J et al. (2018) Diagnosis of LVAD Thrombus using a High-Avidity Fibrin-Specific 99mTc Probe. Theranostics 8:1168-1179
Hathi, Deep K; DeLassus, Elizabeth N; Achilefu, Samuel et al. (2018) Imaging Melphalan Therapy Response in Preclinical Extramedullary Multiple Myeloma with 18F-FDOPA and 18F-FDG PET. J Nucl Med 59:1551-1557
Ghai, Anchal; Maji, Dolonchampa; Cho, Nicholas et al. (2018) Preclinical Development of CD38-Targeted [89Zr]Zr-DFO-Daratumumab for Imaging Multiple Myeloma. J Nucl Med 59:216-222
Ghobadi, Armin; Rettig, Michael P; Holt, Matthew S et al. (2018) Ixazomib, an oral proteasome inhibitor, induces rapid mobilization of hematopoietic progenitor cells in mice. Blood 131:2594-2596

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