Post on 13-Mar-2018
EFFECTIVE HYPOTHERMIC STORAGE OF HUMAN PLURIPOTENT STEM CELL-DERIVED CARDIOMYOCYTES COMPATIBLE WITH GLOBAL DISTRIBUTION OF CELLS FOR CLINICAL
APPLICATIONS AND TOXICOLOGY TESTING Cláudia Correia1,2, Alexey Koshkin1,2, Madalena Carido1,2, Nuno Espinha1,2, Pedro Lima3, Margarida Serra1,2, Paula M Alves1,2
1iBET, Oeiras, Portugal; 2ITQB-UNL, Oeiras, Portugal; 3Nova Medical School, Lisboa, Portugal
AIM ESTABLISHMENT OF EFFECTIVE CLINICALLY COMPATIBLE
STRATEGIES FOR COLD (4ᴼ C) STORAGE OF hPSC-CMS AS 2D MONOLAYERS AND 3D AGGREGATES
The production of cardiomyocytes (CMs) from human pluripotent stem cells (hPSC) holds great promise for patient-specific cardiotoxicity drug testing, disease modeling and cardiac regeneration [1]. The applicability of human pluripotent stem cell-derived cardiomyocytes (hPSC-CMs) in the clinic and industry is highly dependent on the development of efficient methods for worldwide shipment of these cells. We evaluated the feasibility to cold store monolayers and aggregates of functional CMs obtained from different PSC lines using a fully defined clinical-compatible preservation formulation and investigated the time frame that hPSC-CMs could be subjected to hypothermic storage [2].
STRATEGY BACKGROUND
2D MONOLAYERS 3D AGGREGATES
CELL CHARACTERIZATION
HYPOTHERMIC STORAGE
STORAGE SOLUTIONS
STORAGE TIME
MORPHOLOGY STRUCTURE ULTRASTRUCTURE
2D MONOLAYERS
RESULTS
Legend: Nucleus (Nu); myofibrils (MF); Z-bands (Z); neighbouring CMs (CM1, CM2); intercalated disks (ID)
hPSC-CMS WERE STORED FOR 3 (S3), 5 (S5) AND 7 (S7) DAYS AT 4°C IN HYPOTHERMOSOLTM [2]
S7 - Day 1 S7 - Day 7
FD
A / P
I N
UC
VIE
W / M
ITO
VIE
W S7 - Day 1 S7 - Day 7
CELL VIABILITY NECROSIS - FDA (LIVE CELLS) / PI (DEAD CELLS) APOPTOSIS - MITOVIEW (LIVE CELLS)/NUCVIEW (APOPTOTIC CELLS, ACTIVE CASPASE-3)
METABOLIC ACTIVITY RECOVERY PRESTOBLUE ASSAY
HYPOTHERMIC STORAGE OF hPSC-CMS
MF
Z
Z
MF
MF
CM2
CM1
TRANSMISSION ELECTRON MICROSCOPY (TEM)
METABOLOMICS
CULTURE SYSTEM
CELL RECOVERY TRYPAN BLUE ASSAY
3D AGGREGATES
CELL VIABILITY NECROSIS - FDA (LIVE CELLS) / PI (DEAD CELLS)
METABOLIC ACTIVITY RECOVERY PRESTOBLUE ASSAY
SCANNING ELECTRON MICROSCOPY (SEM)
TRANSMISSION ELECTRON MICROSCOPY (TEM)
S7 - Day 7
Legend: Nucleus (Nu); myofibrils (MF); Z-bands (Z); mitochondria (M)
MONOLAYERS OF hPSC-CMS CAN BE EFFICIENTLY COLD STORED FOR 3 DAYS WITHOUT COMPROMISING CELL RECOVERY, METABOLIC ACTIVITY AND ULTRASTRUCTURE
ꭗ CELL VIABILITY DECREASED WHEN THE COLD STORAGE INTERVAL WAS EXTENDED TO 7 DAYS
hPSC-CMS ARE MORE RESISTANT TO PROLONGED HYPOTHERMIC STORAGE-INDUCED CELL INJURY IN 3D AGGREGATES THAN IN 2D MONOLAYERS, SHOWING HIGH CELL RECOVERIES (>70%) AFTER 7 DAYS OF STORAGE
AGGREGATE STRUCTURE/SIZE AND CELL ULTRASTRUCTURE WERE MAINTAINED AFTER 7 DAYS OF STORAGE
1 2 3
0
2 0
4 0
6 0
8 0
1 0 0
S 7 C o n t r o l
B e f o r e S t o r a g e
S I R P A V C A M c T N T
po
si
ti
ve
c
el
ls
(
%)
0 1 2 3 40.0
0.2
0.4
0.6
0.8
1.0
1.2S3 S5 S7
Time post-storage (day)
Fre
qu
en
cy
(in
re
latio
n t
o n
on
-sto
red
ce
lls)
hPSC-CM CHARACTERIZATION FLOW CYTOMETRY
BEATING FREQUENCY
IMMUNOFLUORESCENCE MICROSCOPY
Visit us @ www.ibet.pt Animal Cell Technology Unit, iBET & ITQB-UNL , Portugal Scale-up and Manufacturing of Cell-based Therapies V, January 2017, San Diego, CA, USA
ACKNOWLEDGEMENTS: The authors acknowledge the financial support received from FCT, Portugal (PTDC/BIO/72755/2006), from the European Commission (Hyperlab:223011) and from the FP7 EU project CARE-MI (HEALTH-2009_242038). CC acknowledges the funding from FCT (SFRH/BD/51573/2011).
REFERENCES: [1] Oh, Y., Wei, H., Ma, D., Sun, X. & Liew, R. Clinical applications of patient-specific induced pluripotent stem cells in cardiovascular medicine. Heart 98, 443–9 (2012). [2] Correia, C., Koshkin, A., Carido, M. et al. Effective Hypothermic Storage of Human Pluripotent Stem Cell-Derived
Cardiomyocytes Compatible With Global Distribution of Cells for Clinical Applications and Toxicology Testing. Stem Cells Trans Med. 5;111(3):658-69 (2016).
ELECTROPHYSIOLOGY ANALYSIS
DRUG RESPONSIVENESS
No
rmal
ized
val
ues
N
orm
aliz
ed v
alu
es
CALCIUM TRANSIENTS
AFTER 7 DAYS OF STORAGE, HPSC-CMS MAINTAINED THEIR TYPICAL PROTEIN EXPRESSION PROFILE, SARCOMERIC STRUCTURE, BEATING FREQUENCY, ELECTROPHYSIOLOGICAL PROFILES AND DRUG RESPONSIVENESS
CONCLUSION DEVELOPMENT OF EFFICIENT STRATEGIES FOR
HYPOTHERMIC STORAGE OF 2D MONOLAYERS AND 3D AGGREGATES OF HPSC-CMS
2D MONOLAYER OF HPSC-CMS CAN BE EFFICIENTLY STORED DURING 3 DAYS (80% OF CELL RECOVERY)
3D AGGREGATES OF HPSC-CM PROVIDE BETTER CELL RECOVERY COMPARING TO 2D MONOLAYER AFTER 7 DAYS OF STORAGE
7 DAYS OF HYPOTHERMIC STORAGE DID NOT AFFECT THE PHENOTYPE AND FUNCTION OF HUMAN PSC-CMS STORED EITHER AS MONOLAYERS OR AGGREGATES
STEP FORWARD TOWARDS THE GLOBAL COMMERCIAL DISTRIBUTION OF hPSC-CMS