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. 2024 Aug;26(4):593-602.
doi: 10.1007/s11307-024-01915-z. Epub 2024 May 30.

Tumor Pre-Targeting System Using Streptavidin-Expressing Bacteria

Seong-Young Kwon  1   2 Sung-Hwan You  2   3 Jin Hee Im  1   2 Dinh-Huy Nguyen  2 Dong-Yeon Kim  4 Ayoung Pyo  4 Geun-Joong Kim  5 Hee-Seung Bom  1 Yeongjin Hong  3   6 Jung-Joon Min  7   8   9
Affiliations

Tumor Pre-Targeting System Using Streptavidin-Expressing Bacteria

Seong-Young Kwon et al. Mol Imaging Biol. 2024 Aug.

Abstract

Purpose: A major obstacle to targeted cancer therapy is identifying suitable targets that are specifically and abundantly expressed by solid tumors. Certain bacterial strains selectively colonize solid tumors and can deliver genetically encoded cargo molecules to the tumor cells. Here, we engineered bacteria to express monomeric streptavidin (mSA) in tumors, and developed a novel tumor pre-targeting system by visualizing the presence of tumor-associated mSA using a biotinylated imaging probe.

Procedures: We constructed a plasmid expressing mSA fused to maltose-binding protein and optimized the ribosome binding site sequence to increase solubility and expression levels. E. coli MG1655 was transformed with the recombinant plasmid, expression of which is driven by the pBAD promotor. Expression of mSA was induced by L-arabinose 4 days after injection of bacteria into mice bearing CT26 mouse colon carcinoma cells. Selective accumulation of mSA in tumor tissues was visualized by optical imaging after administration of a biotinylated fluorescent dye. Counting of viable bacterial cells was also performed.

Results: Compared with a conventional system, the novel expression system resulted in significantly higher expression of mSA and sustained binding to biotin. Imaging signals in tumor tissues were significantly stronger in the mSA-expressing group than in non-expressing group (P = 0.0005). Furthermore, the fluorescent signal in tumor tissues became detectable again after multiple inductions with L-arabinose. The bacterial counts in tumor tissues showed no significant differences between conditions with and without L-arabinose (P = 0.45). Western blot analysis of tumor tissues confirmed expression and binding of mSA to biotin.

Conclusions: We successfully engineered tumor-targeting bacteria carrying a recombinant plasmid expressing mSA, which was targeted to, and expressed in, tumor tissues. These data demonstrate the potential of this novel tumor pre-targeting system when combined with biotinylated imaging probes or therapeutic agents.

Keywords: Bacteria; Biotin; Pre-targeting; Streptavidin; Theranostics.

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References

    1. Zhong L, Li Y, Xiong L et al (2021) Small molecules in targeted cancer therapy: advances, challenges, and future perspectives. Signal Transduct Target Ther 6:201 - DOI - PubMed - PMC
    1. Ward RA, Fawell S, Floc’h N, Flemington V, McKerrecher D, Smith PD (2021) Challenges and Opportunities in Cancer Drug Resistance. Chem Rev 121:3297–3351 - DOI - PubMed
    1. Richman SA, Nunez-Cruz S, Moghimi B et al (2018) High-Affinity GD2-Specific CAR T Cells Induce Fatal Encephalitis in a Preclinical Neuroblastoma Model. Cancer Immunol Res 6:36–46 - DOI - PubMed
    1. Leko V, Rosenberg SA (2020) Identifying and Targeting Human Tumor Antigens for T Cell-Based Immunotherapy of Solid Tumors. Cancer Cell 38:454–472 - DOI - PubMed - PMC
    1. Altai M, Membreno R, Cook B, Tolmachev V, Zeglis BM (2017) Pretargeted Imaging and Therapy. J Nucl Med 58:1553–1559 - DOI - PubMed - PMC

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