Author
Listed:
- Nalinikanth Kotagiri
(Washington University School of Medicine
University of Cincinnati)
- Matthew L. Cooper
(Washington University School of Medicine)
- Michael Rettig
(Washington University School of Medicine)
- Christopher Egbulefu
(Washington University School of Medicine)
- Julie Prior
(Washington University School of Medicine)
- Grace Cui
(Washington University School of Medicine)
- Partha Karmakar
(Washington University School of Medicine)
- Mingzhou Zhou
(Washington University School of Medicine)
- Xiaoxia Yang
(Washington University School of Medicine)
- Gail Sudlow
(Washington University School of Medicine)
- Lynne Marsala
(Washington University School of Medicine)
- Chantiya Chanswangphuwana
(Washington University School of Medicine)
- Lan Lu
(Washington University School of Medicine)
- LeMoyne Habimana-Griffin
(Washington University School of Medicine)
- Monica Shokeen
(Washington University School of Medicine)
- Xinming Xu
(Washington University School of Medicine)
- Katherine Weilbaecher
(Washington University School of Medicine)
- Michael Tomasson
(Washington University School of Medicine)
- Gregory Lanza
(Washington University School of Medicine)
- John F. DiPersio
(Washington University School of Medicine)
- Samuel Achilefu
(Washington University School of Medicine
Washington University School of Medicine
Washington University)
Abstract
Most cancer patients succumb to disseminated disease because conventional systemic therapies lack spatiotemporal control of their toxic effects in vivo, particularly in a complicated milieu such as bone marrow where progenitor stem cells reside. Here, we demonstrate the treatment of disseminated cancer by photoactivatable drugs using radiopharmaceuticals. An orthogonal-targeting strategy and a contact-facilitated nanomicelle technology enabled highly selective delivery and co-localization of titanocene and radiolabelled fluorodeoxyglucose in disseminated multiple myeloma cells. Selective ablation of the cancer cells was achieved without significant off-target toxicity to the resident stem cells. Genomic, proteomic and multimodal imaging analyses revealed that the downregulation of CD49d, one of the dimeric protein targets of the nanomicelles, caused therapy resistance in small clusters of cancer cells. Similar treatment of a highly metastatic breast cancer model using human serum albumin-titanocene formulation significantly inhibited cancer growth. This strategy expands the use of phototherapy for treating previously inaccessible metastatic disease.
Suggested Citation
Nalinikanth Kotagiri & Matthew L. Cooper & Michael Rettig & Christopher Egbulefu & Julie Prior & Grace Cui & Partha Karmakar & Mingzhou Zhou & Xiaoxia Yang & Gail Sudlow & Lynne Marsala & Chantiya Cha, 2018.
"Radionuclides transform chemotherapeutics into phototherapeutics for precise treatment of disseminated cancer,"
Nature Communications, Nature, vol. 9(1), pages 1-12, December.
Handle:
RePEc:nat:natcom:v:9:y:2018:i:1:d:10.1038_s41467-017-02758-9
DOI: 10.1038/s41467-017-02758-9
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