The Anterior Eye Chamber as a Visible Medium for In Vivo Tumorigenicity Tests

Author:

Inagaki Emi123,Arai Eri4,Hatou Shin35,Sayano Tomoko35,Taniguchi Hiroko3,Negishi Kazuno3,Kanai Yae4,Sato Yasunori6,Okano Hideyuki1,Tsubota Kazuo3,Shimmura Shigeto3ORCID

Affiliation:

1. Department of Physiology, Keio University School of Medicine , Tokyo , Japan

2. Japanese Society for the Promotion of Science (JSPS) , Tokyo , Japan

3. Department of Ophthalmology, Keio University School of Medicine , Tokyo , Japan

4. Department of Pathology, Keio University School of Medicine , Tokyo , Japan

5. Cellusion Inc. , Tokyo , Japan

6. Department of Preventive Medicine and Public Health, Keio University School of Medicine , Tokyo , Japan

Abstract

Abstract Pluripotent stem cell (PSC)-based cell therapies have increased steadily over the past few years, and assessing the risk of tumor formation is a high priority for clinical studies. Current in vivo tumorigenesis studies require several months and depend strongly on the site of grafting. In this study, we report that the anterior eye chamber is preferable to the subcutaneous space for in vivo tumorigenesis studies for several reasons. First, cells can easily be transplanted into the anterior chamber and monitored in real-time without sacrificing the animals due to the transparency of the cornea. Second, tumor formation is faster than with the conventional subcutaneous method. The median tumor formation time in the subcutaneous area was 18.50 weeks (95% CI 10.20-26.29), vs. 4.0 weeks (95% CI 3.34-.67) in the anterior chamber (P = .0089). When hiPSCs were spiked with fibroblasts, the log10TPD50 was 3.26, compared with 4.99 when hiPSCs were transplanted without fibroblasts. There was more than a 40-fold difference in the log10TPD50 values with fibroblasts. Furthermore, the log10TPD50 for HeLa cells was 1.45 and 100% of animals formed tumors at a concentration greater than 0.1%, indicating that the anterior chamber tumorigenesis assays can be applied for cancer cell lines as well. Thus, our method has the potential to become a powerful tool in all areas of tumorigenesis studies and cancer research.

Publisher

Oxford University Press (OUP)

Subject

Cell Biology,Developmental Biology,General Medicine

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