A first-in-human clinical study of an allogenic iPSC-derived corneal endothelial cell substitute transplantation for bullous keratopathy

Masatoshi Hirayama; Shin Hatou; Masaki Nomura; Risa Hokama; Osama Ibrahim Hirayama; Emi Inagaki; Kumi Aso; Tomoko Sayano; Hiromi Dohi; Tadaaki Hanatani; Naoko Takasu; Hideyuki Okano; Kazuno Negishi; Shigeto Shimmura

doi:10.1016/j.xcrm.2024.101847

A first-in-human clinical study of an allogenic iPSC-derived corneal endothelial cell substitute transplantation for bullous keratopathy

Masatoshi Hirayama, Shin Hatou, Masaki Nomura, Risa Hokama, Osama Ibrahim Hirayama, Emi Inagaki, Kumi Aso, Tomoko Sayano, Hiromi Dohi, Tadaaki Hanatani, Naoko Takasu, Hideyuki Okano, Kazuno Negishi, Shigeto Shimmura

Department of Clinical Regenerative Medicine

Research output: Contribution to journal › Article › peer-review

Abstract

A first-in-human investigator-initiated clinical study of a corneal endothelial cell substitute (CLS001) derived from a clinical-grade induced pluripotent stem cell (iPSC) line shows improvement of visual acuity and corneal stromal edema, with no adverse events for up to 1 year after surgery for the treatment of bullous keratopathy. While preclinical tests, including multiple whole-genome analysis and tumorigenicity tests adhering to the Food and Drug Administration (FDA) draft guidelines, are negative, an additional whole-genome analysis conducted on transplanted CLS001 cells reveals a de novo in-frame deletion of exon22 in the EP300 gene. No adverse events related to the mutation are observed. Our study demonstrates the feasibility of using iPSC-derived cells to replace donor transplant for bullous keratopathy, while shedding light on risk management of gene mutation in cell products. Further follow-up is required for long-term analysis of clinical safety and efficacy.

Original language	English
Article number	101847
Journal	Cell Reports Medicine
Volume	6
Issue number	1
DOIs	https://doi.org/10.1016/j.xcrm.2024.101847
Publication status	Published - 21-01-2025

All Science Journal Classification (ASJC) codes

General Biochemistry,Genetics and Molecular Biology

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Hirayama, M., Hatou, S., Nomura, M., Hokama, R., Hirayama, O. I., Inagaki, E., Aso, K., Sayano, T., Dohi, H., Hanatani, T., Takasu, N., Okano, H., Negishi, K., & Shimmura, S. (2025). A first-in-human clinical study of an allogenic iPSC-derived corneal endothelial cell substitute transplantation for bullous keratopathy. Cell Reports Medicine, 6(1), Article 101847. https://doi.org/10.1016/j.xcrm.2024.101847

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title = "A first-in-human clinical study of an allogenic iPSC-derived corneal endothelial cell substitute transplantation for bullous keratopathy",

abstract = "A first-in-human investigator-initiated clinical study of a corneal endothelial cell substitute (CLS001) derived from a clinical-grade induced pluripotent stem cell (iPSC) line shows improvement of visual acuity and corneal stromal edema, with no adverse events for up to 1 year after surgery for the treatment of bullous keratopathy. While preclinical tests, including multiple whole-genome analysis and tumorigenicity tests adhering to the Food and Drug Administration (FDA) draft guidelines, are negative, an additional whole-genome analysis conducted on transplanted CLS001 cells reveals a de novo in-frame deletion of exon22 in the EP300 gene. No adverse events related to the mutation are observed. Our study demonstrates the feasibility of using iPSC-derived cells to replace donor transplant for bullous keratopathy, while shedding light on risk management of gene mutation in cell products. Further follow-up is required for long-term analysis of clinical safety and efficacy.",

keywords = "bullous keratopathy, cell therapy, cornea, gene mutation, induced pluripotent stem cells, transplantation",

author = "Masatoshi Hirayama and Shin Hatou and Masaki Nomura and Risa Hokama and Hirayama, {Osama Ibrahim} and Emi Inagaki and Kumi Aso and Tomoko Sayano and Hiromi Dohi and Tadaaki Hanatani and Naoko Takasu and Hideyuki Okano and Kazuno Negishi and Shigeto Shimmura",

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Hirayama, M, Hatou, S, Nomura, M, Hokama, R, Hirayama, OI, Inagaki, E, Aso, K, Sayano, T, Dohi, H, Hanatani, T, Takasu, N, Okano, H, Negishi, K & Shimmura, S 2025, 'A first-in-human clinical study of an allogenic iPSC-derived corneal endothelial cell substitute transplantation for bullous keratopathy', Cell Reports Medicine, vol. 6, no. 1, 101847. https://doi.org/10.1016/j.xcrm.2024.101847

TY - JOUR

T1 - A first-in-human clinical study of an allogenic iPSC-derived corneal endothelial cell substitute transplantation for bullous keratopathy

AU - Hirayama, Masatoshi

AU - Hatou, Shin

AU - Nomura, Masaki

AU - Hokama, Risa

AU - Hirayama, Osama Ibrahim

AU - Inagaki, Emi

AU - Aso, Kumi

AU - Sayano, Tomoko

AU - Dohi, Hiromi

AU - Hanatani, Tadaaki

AU - Takasu, Naoko

AU - Okano, Hideyuki

AU - Negishi, Kazuno

AU - Shimmura, Shigeto

PY - 2025/1/21

Y1 - 2025/1/21

N2 - A first-in-human investigator-initiated clinical study of a corneal endothelial cell substitute (CLS001) derived from a clinical-grade induced pluripotent stem cell (iPSC) line shows improvement of visual acuity and corneal stromal edema, with no adverse events for up to 1 year after surgery for the treatment of bullous keratopathy. While preclinical tests, including multiple whole-genome analysis and tumorigenicity tests adhering to the Food and Drug Administration (FDA) draft guidelines, are negative, an additional whole-genome analysis conducted on transplanted CLS001 cells reveals a de novo in-frame deletion of exon22 in the EP300 gene. No adverse events related to the mutation are observed. Our study demonstrates the feasibility of using iPSC-derived cells to replace donor transplant for bullous keratopathy, while shedding light on risk management of gene mutation in cell products. Further follow-up is required for long-term analysis of clinical safety and efficacy.

AB - A first-in-human investigator-initiated clinical study of a corneal endothelial cell substitute (CLS001) derived from a clinical-grade induced pluripotent stem cell (iPSC) line shows improvement of visual acuity and corneal stromal edema, with no adverse events for up to 1 year after surgery for the treatment of bullous keratopathy. While preclinical tests, including multiple whole-genome analysis and tumorigenicity tests adhering to the Food and Drug Administration (FDA) draft guidelines, are negative, an additional whole-genome analysis conducted on transplanted CLS001 cells reveals a de novo in-frame deletion of exon22 in the EP300 gene. No adverse events related to the mutation are observed. Our study demonstrates the feasibility of using iPSC-derived cells to replace donor transplant for bullous keratopathy, while shedding light on risk management of gene mutation in cell products. Further follow-up is required for long-term analysis of clinical safety and efficacy.

KW - bullous keratopathy

KW - cell therapy

KW - cornea

KW - gene mutation

KW - induced pluripotent stem cells

KW - transplantation

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A first-in-human clinical study of an allogenic iPSC-derived corneal endothelial cell substitute transplantation for bullous keratopathy

Abstract

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