Bridging the organoid translational gap: integrating standardization and micropatterning for drug screening in clinical and pharmaceutical medicine

Author:

Yang Haowei12,Li Jiawei12,Wang Zitian1,Khutsishvili Davit1,Tang Jiyuan1,Zhu Yu3,Cai Yongde1,Dai Xiaoyong1,Ma Shaohua124ORCID

Affiliation:

1. Tsinghua Shenzhen International Graduate School (SIGS), Tsinghua University , Shenzhen 518055 , China

2. Tsinghua-Berkeley Shenzhen Institute , Shenzhen 518055 , China

3. Guangdong Research Center of Organoid Engineering and Technology , Guangzhou 510530 , China

4. Key Laboratory of Industrial Biocatalysis (Ministry of Education), Tsinghua University , Beijing 100084 , China

Abstract

Abstract Synthetic organ models such as organoids and organ-on-a-chip have been receiving recognition from administrative agencies. Despite the proven success of organoids in predicting drug efficacy on laboratory scales, their translational advances have not fully satisfied the expectations for both clinical implementation and commercial applications. The transition from laboratory settings to clinical applications continues to encounter challenges. Employing engineering methodologies to facilitate the bridging of this gap for organoids represents one of the key directions for future advancement. The main measures to bridge the gap include environmental and phenotypic recapitulation, 3D patterning, matrix engineering, and multi-modality information acquisition and processing. Pilot whole-process clinical/pharmaceutical applications with fast and standardized organoid models will continuously offer convincing frontline optimization clues and driving forces to the organoid community, which is a promising path to translational organoid technologies.

Publisher

Oxford University Press (OUP)

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