Label‐Free Impedance Analysis of Induced Pluripotent Stem Cell‐Derived Spinal Cord Progenitor Cells for Rapid Safety and Efficacy Profiling

Author:

He Linwei1ORCID,Tan Jerome234ORCID,Ng Shi Yan5ORCID,Li King Ho Holden1ORCID,Han Jongyoon467ORCID,Chew Sing Yian2489ORCID,Hou Han Wei148ORCID

Affiliation:

1. School of Mechanical and Aerospace Engineering Nanyang Technological University 50 Nanyang Avenue Singapore 639798 Singapore

2. School of Chemistry, Chemical Engineering and Biotechnology Nanyang Technological University 62 Nanyang Drive Singapore 637459 Singapore

3. NTU Institute of Health Technologies Interdisciplinary Graduate Programme Nanyang Technological University 61 Nanyang Drive Singapore 637335 Singapore

4. Critical Analytics for Manufacturing of Personalized Medicine IRG Singapore‐MIT Alliance for Research and Technology Centre 1 Create Way Singapore 138602 Singapore

5. Institute of Molecular and Cell Biology Agency for Science, Technology and Research (A*STAR) Research Entities 61 Biopolis Drive, Proteos Singapore 138673 Singapore

6. Department of Biological Engineering Massachusetts Institute of Technology 21 Ames St Cambridge MA 02139 USA

7. Department of Electrical Engineering and Computer Science Massachusetts Institute of Technology 50 Vassar St Cambridge MA 02139 USA

8. Lee Kong Chian School of Medicine Nanyang Technological University 59 Nanyang Drive Singapore 636921 Singapore

9. School of Materials Science and Engineering Nanyang Technological University 50 Nanyang Ave Singapore 639798 Singapore

Abstract

AbstractRegenerative therapies, including the transplantation of spinal cord progenitor cells (SCPCs) derived from induced pluripotent stem cells (iPSCs), are promising treatment strategies for spinal cord injuries. However, the risk of tumorigenicity from residual iPSCs advocates an unmet need for rapid SCPCs safety profiling. Herein, a rapid (≈3000 cells min‐1) electrical‐based microfluidic biophysical cytometer is reported to detect low‐abundance iPSCs from SCPCs at single‐cell resolution. Based on multifrequency impedance measurements (0.3 to 12 MHz), biophysical features including cell size, deformability, membrane, and nucleus dielectric properties are simultaneously quantified as a cell is hydrodynamically stretched at a cross junction under continuous flow. A supervised uniform manifold approximation and projection (UMAP) model is further developed for impedance‐based quantification of undifferentiated iPSCs with high sensitivity (≈1% spiked iPSCs) and shows good correlations with SCPCs differentiation outcomes using two iPSC lines. Cell membrane opacity (day 1) is also identified as a novel early intrinsic predictive biomarker that exhibits a strong correlation with SCPC differentiation efficiency (day 10). Overall, it is envisioned that this label‐free and optic‐free platform technology can be further developed as a versatile cost‐effective process analytical tool to monitor or assess stem cell quality and safety in regenerative medicine. 

Funder

National Research Foundation Singapore

Ministry of Education - Singapore

Publisher

Wiley

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