Efficacy of Tumor-Targeting Salmonella typhimurium A1-R against Malignancies in Patient-Derived Orthotopic Xenograft (PDOX) Murine Models
Abstract
:1. Introduction
2. S. typhimurium A1-R against PDOX Tumor Models
2.1. Overview
2.2. Establishment of PDOX Models
2.3. S. typhimurium A1-R Therapy
2.4. S. typhimurium A1-R Treatment Efficacies
2.4.1. Tumor-Targeting Efficacy
2.4.2. Antitumor Efficacy of S. typhimurium A1-R Compared to Untreated Control
2.4.3. Antitumor Efficacy of S. typhimurium A1-R Compared to Chemotherapy or Molecular-Targeting Therapy
2.4.4. Synergistic Antitumor Efficacy of S. typhimurium A1-R in Combination with Other Agents
2.4.5. Histological Effects
2.5. Adverse Effects Caused by S. typhimurium A1-R Treatment
3. Conclusions and Future Perspectives
Author Contributions
Funding
Conflicts of Interest
Dedication
References
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Patient | Mouse | ||||
---|---|---|---|---|---|
Tumor Type (Subtype) | Year | Origin | Original Site | Genetics | Implanted Site |
Pancreatic Cancer | |||||
2014 [23] | Primary | Pancreas | VEGF+ | Pancreas | |
2014 [24] | Primary | Pancreas | - | Pancreas | |
2018 [36] | Primary | Pancreas | - | Pancreas | |
Soft Tissue Sarcoma | |||||
(FDCS) | 2016 [25] | Recurrent/regional | Lower extremity (Primary site: lower extremity) | - | Lower extremity |
(UPS) | 2016 [27] | Primary | Lower extremity | - | Lower extremity |
(Ewing’s sarcoma) | 2017 [28] | Primary | Chest wall | - | Chest wall |
(Pleomorphic liposarcoma) | 2018 [33] | Recurrent/regional | Upper extremity (Primary site: upper extremity) | PDGFRA amplification | Upper extremity |
(USTS) | 2018 [37] | Primary | Lower extremity | - | Lower extremity |
(Myxofibrosarcoma) | 2018 [39] | Recurrent/regional | Upper extremity | - | Upper extremity |
Melanoma | |||||
2016 [26] | Primary | Chest wall | BRAF-V600E mutation | Chest wall | |
2017 [29] | Primary | Chest wall | BRAF-V600E mutation | Chest wall | |
2017 [30] | Primary | Chest wall | BRAF-V600E mutation | Chest wall | |
2018 [34] | Primary | Abdominal wall | BRAF-V600E mutation negative | Abdominal wall | |
Osteosarcoma | |||||
2017 [31] | Recurrent/distant | Lung (Primary site: femur) | - | Femur | |
2018 [35] | Recurrent/distant | Lung (Primary site: femur) | - | Lung | |
GIST | |||||
2018 [32] | Recurrent/regional | Lymph node (Primary site: stomach) | c-kit (exon 11 and 17) mutation | Gastric wall | |
Cancer of Unknown Primary | |||||
2018 [38] | Metastatic | Neck lymph node (Primary site: unknown) | - | Left supraclavicular fossa |
S. typhimurium A1-R | ||||
---|---|---|---|---|
Tumor Type (Subtype) | Route | Dose | Mono- or Polytherapy | Antitumor Effect |
Pancreatic Cancer | ||||
[23] | i.v. | 5 × 107 CFU | Polytherapy | BEV + GEM → A1-R > BEV + GEM > GEM > Ct |
[24] | i.p. | 1.5 × 108 CFU | Monotherapy | A1-R > GEM or CDDP or 5FU > Ct |
[36] | i.v. | 5 × 107 CFU | Monotherapy Polytherapy | A1-R > Ct A1-R + GEM > A1-R or GEM + nPTX or GEM or Ct |
Soft Tissue Sarcoma | ||||
(FDCS) [25] | i.p. | 2 × 107 CFU | Monotherapy Polytherapy | A1-R > Ct A1-R → DOX > Ct, A1-R → BEZ > Ct |
(UPS) [27] | i.t. | 5 × 107 CFU | Monotherapy Polytherapy | A1-R > Ct A1-R → DOX > Ct |
(Ewing’s sarcoma) [28] | i.v./i.t. | 5 × 107 CFU | Monotherapy Polytherapy | A1-R > Ct A1-R + DOX > Ct |
(Pleomorphic liposarcoma) [33] | i.v. | 5 × 107 CFU | Monotherapy | A1-R > DOX or Ct |
(USTS) [37] | i.v. | 5 × 107 CFU | Monotherapy | A1-R > DOX > Ct |
(Myxofibrosarcoma) [39] | i.v. | 5 × 107 CFU | Monotherapy | A1-R > DOX or Ct |
Melanoma | ||||
[26] | i.v. | 5 × 107 CFU | Monotherapy Polytherapy | A1-R > Ct A1-R + TEM > A1-R, A1-R + TEM > TEM |
[29] | i.v. | 5 × 107 CFU | Monotherapy Polytherapy | A1-R > Ct A1-R + TEM or A1-R + VEM > A1-R |
[30] | i.v. | 5 × 107 CFU | Monotherapy Polytherapy | A1-R > Ct A1-R + VEM > COB + VEM or COB or VEM or A1-R or Ct |
[34] | i.v. | 5 × 107 CFU | Monotherapy Polytherapy | A1-R > Ct A1-R + rMETase > TEM + rMETase or rMETase or TEM or Ct |
Osteosarcoma | ||||
[31] | i.v/i.a. | 5 × 107 CFU (i.v.) 5 × 105 CFU (i.a.) | Monotherapy | A1-R (i.a.) > A1-R (i.v.) or CDDP or Ct, A1-R (i.v.) > Ct |
[35] | i.v. | 5 × 107 CFU | Monotherapy Polytherapy | A1-R > CDDP or Ct A1-R + rMETase + CDDP > A1-R + rMETase > A1-R or rMETase or CDDP or Ct |
GIST | ||||
[32] | i.v. | 5 × 107 CFU | Monotherapy | A1-R > IMA or Ct |
Cancer of Unknown Primary | ||||
[38] | i.v. | 5 × 107 CFU | Monotherapy | A1-R > Ct |
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Share and Cite
Murakami, T.; Hiroshima, Y.; Miyake, K.; Kiyuna, T.; Endo, I.; Zhao, M.; Hoffman, R.M. Efficacy of Tumor-Targeting Salmonella typhimurium A1-R against Malignancies in Patient-Derived Orthotopic Xenograft (PDOX) Murine Models. Cells 2019, 8, 599. https://doi.org/10.3390/cells8060599
Murakami T, Hiroshima Y, Miyake K, Kiyuna T, Endo I, Zhao M, Hoffman RM. Efficacy of Tumor-Targeting Salmonella typhimurium A1-R against Malignancies in Patient-Derived Orthotopic Xenograft (PDOX) Murine Models. Cells. 2019; 8(6):599. https://doi.org/10.3390/cells8060599
Chicago/Turabian StyleMurakami, Takashi, Yukihiko Hiroshima, Kentaro Miyake, Tasuku Kiyuna, Itaru Endo, Ming Zhao, and Robert M. Hoffman. 2019. "Efficacy of Tumor-Targeting Salmonella typhimurium A1-R against Malignancies in Patient-Derived Orthotopic Xenograft (PDOX) Murine Models" Cells 8, no. 6: 599. https://doi.org/10.3390/cells8060599
APA StyleMurakami, T., Hiroshima, Y., Miyake, K., Kiyuna, T., Endo, I., Zhao, M., & Hoffman, R. M. (2019). Efficacy of Tumor-Targeting Salmonella typhimurium A1-R against Malignancies in Patient-Derived Orthotopic Xenograft (PDOX) Murine Models. Cells, 8(6), 599. https://doi.org/10.3390/cells8060599