Production and nonclinical evaluation of an autologous iPSC-derived platelet product for the iPLAT1 clinical trial

用于 iPLAT1 临床试验的自体 iPSC 衍生血小板产品的生产和非临床评估

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作者:Naoshi Sugimoto ,Sou Nakamura ,Shin Shimizu ,Akiko Shigemasa ,Junya Kanda ,Nobuki Matsuyama ,Mitsunobu Tanaka ,Tomoya Hayashi ,Akihiro Fuchizaki ,Masayuki Nogawa ,Naohide Watanabe ,Shinichiro Okamoto ,Makoto Handa ,Akira Sawaguchi ,Dai Momose ,Ki-Ryang Koh ,Yoshihiko Tani ,Akifumi Takaori-Kondo ,Koji Eto

Abstract

Donor-derived platelets are used to treat or prevent hemorrhage in patients with thrombocytopenia. However, ∼5% or more of these patients are complicated with alloimmune platelet transfusion refractoriness (allo-PTR) due to alloantibodies against HLA-I or human platelet antigens (HPA). In these cases, platelets from compatible donors are necessary, but it is difficult to find such donors for patients with rare HLA-I or HPA. To produce platelet products for patients with aplastic anemia with allo-PTR due to rare HPA-1 mismatch in Japan, we developed an ex vivo good manufacturing process (GMP)-based production system for an induced pluripotent stem cell-derived platelet product (iPSC-PLTs). Immortalized megakaryocyte progenitor cell lines (imMKCLs) were established from patient iPSCs, and a competent imMKCL clone was selected for the master cell bank (MCB) and confirmed for safety, including negativity of pathogens. From this MCB, iPSC-PLTs were produced using turbulent flow bioreactors and new drugs. In extensive nonclinical studies, iPSC-PLTs were confirmed for quality, safety, and efficacy, including hemostasis in a rabbit model. This report presents a complete system for the GMP-based production of iPSC-PLTs and the required nonclinical studies and thus supports the iPLAT1 study, the first-in-human clinical trial of iPSC-PLTs in a patient with allo-PTR and no compatible donor using the autologous product. It also serves as a comprehensive reference for the development of widely applicable allogeneic iPSC-PLTs and other cell products that use iPSC-derived progenitor cells as MCB.

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