Progress in clinical applications of PSCs in 2017 Trounson A. et al. Nature Reviews Molecular Cell Biology 17, 194–200 (2016) doi:10.1038/nrm.2016.10 Robust strategies have been developed to differentiate pluripotent stem cells into retinal pigment epithelium, A9 dopaminergic neurons, oligodendrocyte, pancreatic βislet cells and cardiomyocytes. Clinical trials are underway for embryonic stem cell (ES cell) derivatives for age-related macular degeneration (AMD), type I diabetes, spinal cord injury, myocardial infarct and Parkinson disease (using parthenogenetic embryonic stem cells (pES cells)). Induced pluripotent stem cells (iPSCs) are in a clinical trial for AMD. Rigorously tested, abundant sources of these cell types are needed for preclinical research to generate data for regulatory approval for human studies. The cells also need to be manufactured in large quantities for clinical trials. These clinical studies in humans begin with regulatory approval for Phase I trials, which demonstrate safety. They are followed by Phase II studies showing proof of concept for cell therapy in human patients. Sometimes, Phase I–II studies are designed to demonstrate both safety and efficacy. Larger-scale Phase III clinical trials aim to demonstrate the statistical significance of the therapeutic benefit. The bench to bedside pathway Knoepfler PS Adv Drug Deliv Rev. 2015 Mar;82-83:192-6. Diagram of the evolving clinical trials process and other mechanisms of therapy translation to the bedside. The traditional, multi-phasic FDA clinical trials process is shown in black with a black arrow from bench to bedside. Evolving FDA mechanisms for accelerating the clinical trial process are shown in orange. Compassionate Use (also known as “Expanded Access”) and Right To Try (RTT) are shown in green with a loop reflecting the bypassing of Phase 2 and Phase 3. It is notable that the requirements for Compasionate Use are evolving and there are diverse stakeholder views. The precise pre-requisites (e.g. Phase 1 versus Phase 2 data) obtainable from FDA guidance are not completely clear and may vary on a case-by-case basis. The common stem cell clinic approach of entirely avoiding the clinical trials approval process is shown in red. Note that for some non-more than minimally manipulated stem cell products used in a homologous manner, direct use by stem cell clinics or other physicians may be appropriate with only a relatively minor role for the FDA. • 41,054 studies (total) • • 28849 studies: heart, cardiac, coronary • 6240 studies : heart failure • 210 studies: heart failure stem cell • 4 studies: heart human embryonic • 4 studies: heart human induced pluripotent • 1 study: heart failure induced pluripotent - diagnostic https://clinicaltrials.gov/ct2/results?term=heart+failure+human+embryonic https://clinicaltrials.gov/ct2/show/NCT02057900?term=heart+failure+human+embryoni c&rank=1 PATCH http://www.onlinejacc.org/highwire/markup/28281/expansion?width=1000&height=50 0&iframe=true&postprocessors=highwire_figures%2Chighwire_math%2Chighwire_inlin e_linked_media%2Chighwire_embed https://clinicaltrials.gov/ct2/results?term=heart+human+induced+pluripotent&type=&r slt=&recr=&age_v=&gndr=&cond=&intr=&titles=&outc=&spons=&lead=&id=&state1=& cntry1=&state2=&cntry2=&state3=&cntry3=&locn=&rcv_s=&rcv_e=&lup_s=&lup_e= Why? • human heart has limited potential for regeneration, the loss of cardiomyocytes during course of cardio-myopathy and ischaemic injury can result in heart failure and death What to do? • current status – prevention – non smoking, education, lifestyle, lipids… – AC Inhibitor – lowe blood pressure, reverse remodeling – Betablocker – reduces adrenergic stimulation = lower oxygen consumption / need – Diuretics – reduces volume overload – etc… symptomatic treatment – Bypass / Angioplasty / Transplantation… in time? • cardiac repair is strategy to regenerate functionally viable myocardium after insult as myocardial infarction to prevent or heal heart failure… How? • cells/ tissues / vessels • growth factors / cytokines • origin: endogenouse repair– original tissue autologouse – other organs allogenic – other human(s) xenogenic – other species • number of different strategies… Bosniak Z. 3rd Dubrovni Cardiology Highlihts lecture Source ? –– Sanganalmath S Bolli R Circ Res. 2013 Aug 30; 113(6): 810–834. Skeletal Myoblasts? • precursors of satellite cells (SKMs) • muscle biopsies, proliferative + resistant to ischaemia and hypoxia • no functional coupling of SKMs with the myocardium in vivo = fail to contract synchronously with the native myocardium • the MAGIC trial - no significant improvement in LV function = discontinued P. Menasch´e, O. Alfieri, S. Janssens et al., “The myoblast autologous grafting in ischemic cardiomyopathy (MAGIC) trial: first randomized placebo-controlled study of myoblast transplantation,” Circulation, vol. 117, no. 9, pp. 1189–1200, 2008. [41] H. Reinecke, V. Poppa, and C. E. Murry, “Skeletal muscle stem cells do not transdifferentiate into cardiomyocytes after cardiac grafting,” Journal of Molecular and Cellular Cardiology, vol. 34, no. 2, pp. 241–249, 2002. Bone Marrow-Derived Stem Cells (BMCs) unselected ? • in circulation- contribute to myocytes renewal (cell fusion and transdifferentiation) haematopoietic stem cells (HSCs) mesenchymal stem cells (MSCs) endothelial progenitor cells (EPCs) - is optimal the mixture of stem-like cells ? • harvested from pelvic bones of patients • TheTOPCARE-AMI, • BALANCE trial - intracoronary BMMNCs showed 10-11% inc. LVEF (5Y) • meta- analysis: over 3000 patients have been treated with BMCs – overall LVEF (+3.96%) – smaller infarct size ( −4.03%) – clinical significance? – limited data on mortality, recurrence of MI, and rehospitalization for heart failure – no of carcinogenesis, arrhythmias, or any other adverse effects D. M. Leistner, U. Fischer-Rasokat, J. Honold et al., “Transplantation of progenitor cells and regeneration enhancement in acute myocardial infarction (TOPCARE-AMI): final 5-year results suggest long-term safety and efficacy,” Clinical Research in Cardiology, vol. 100, no. 10, pp. 925–934, 2011. M. Yousef, C.M. Schannwell, M. K¨ostering, T. Zeus, M. Brehm, and B. E. Strauer, “The BALANCE Study: clinical benefit and long-term outcome after intracoronary autologous bone marrow cell transplantation in patients with acute myocardial infarction,” Journal of the American College of Cardiology, vol. 53, no. 24, pp. 2262–2269, 2009. Bone Marrow-Derived Stem Cells clinical trial in Brno Long-term results of intracoronary bone marrow cell transplantation: the potential of gated sestamibi SPECT/FDG PET imaging to select patients with maximum benefit from cell therapy. Kaminek M, Meluzin J, Panovský R, Metelkova I, Budikova M, Richter M. Clin Nucl Med. 2010 Oct;35(10):780-7. doi: 10.1097/RLU.0b013e3181e4d9c5. Autologous transplantation of mononuclear bone marrow cells in patients with acute myocardial infarction: the effect of the dose of transplanted cells on myocardial function. Meluzín J, Mayer J, Groch L, Janousek S, Hornácek I, Hlinomaz O, Kala P, Panovský R, Prásek J, Kamínek M, Stanícek J, Klabusay M, Korístek Z, Navrátil M, Dusek L, Vinklárková J. Am Heart J. 2006 Nov;152(5):975.e9-15. Mesenchymal Stem Cells (MSCs) selected? • Bone Marrow - LVEF was increased by approximately 6.7% at 6 months, an inverse dose response, 20 million better than 200 million cells, - the POSEIDON-pilot • Umbilical cord matrix in 18-month follow-up, global LVEF improved by 5% no arrhythmias or immuno side effects • Adipose-Derived Mesenchymal Stem Cells. harvested and expanded o MHC class II antigens, differentiate in to cardiomyocytes and endothelial cells upon induction the PRECISE study cells stabilized the scar size in patients with advanced ischaemic heart disease (not reduction of scar size or increase LVEF) J. M. Hare, J. E. Fishman, G. Gerstenblith et al., “Comparison of allogeneic vs autologous bonemarrow-derivedmesenchymal stem cells delivered by transendocardial injection in patients with ischemic cardiomyopathy: the POSEIDON randomized trial,” JAMA, vol. 308, no. 22, pp. 2369–2379, 2012. The TRansendocardial Stem Cell Injection Delivery Effects on Neomyogenesis STudy (The TRIDENT Study) (Trident) (NCT02013674) E. C. Perin, R. Sanz-Ruiz, P. L. S´anchez et al., “Adipose-derived regenerative cells in patients with ischemic cardiomyopathy: the PRECISE Trial,” American Heart Journal, vol. 168, no. 1, pp. 88.e2–95.e2, 2014. Cardiac Stem Cells (CSCs )? • resident stem-like cells, self-renewing cells able to differentiate into a 3 cell lineages • low proportion (0.01%) of native cardiomyocytes = low turnover rate • meta-analysis 1970 animals improvement in LVEF by approximately 12% • SCIPIO study phase I, c-kit+ CSCs - ischaemic MI, CSCs from right atrial appendage CABG – 1 million of cells administered to 16 patients intracoronary 4 months after CABG increase in LVEF 12.3% at 12 months injection / no tumour formation – 4–8% of transplanted CSCs colonized / persisted in the myocardium 1y – effect of paracrine factors released by injected cells modulating the proliferation of the host cardiac cells? R. Bolli, A. R. Chugh, D. D’Amario et al., “Cardiac stem cells in patients with ischaemic cardiomyopathy (SCIPIO): initial results of a randomised phase 1 trial,” The Lancet, vol. 378, no. 9806, pp. 1847–1857, 2011. Cardiosphere-Derived Cells (CSps)? • in vitro cultured myocardial biopsies form spheroids • self-renewal, positive for progenitor cell markers (c-kit, CD-34, Sca-1, and Nkx2.5) • heterogeneous mixture of cardiac stem cells, differentiating progenitors and differentiated cardiomyocytes • enhance cardiac function, angiogenic formation, and paracrine factor secretion (supporting cells) • the CADUCEUS - decreased scar size of 12.3% at 12 months - no improvement in global LVEF • large size may embolize capillary • lack MHC II antigen = allogeneic CDCs trials R. R. Makkar, R. R. Smith, K. Cheng et al., “Intracoronary cardiosphere-derived cells for heart regeneration after myocardial infarction (CADUCEUS): a prospective, randomised phase 1 trial,” The Lancet, vol. 379, no. 9819, pp. 895–904, 2012. Embryonic Stem Cells (ESCs)? • derived from the inner cell mass of the early embryo in the blastocyst stage • self-renewing, clonogenic, and capable of differentiating into any type of cell in the adult • atrial-like, ventricular-like, sinus nodal-like, Purkinje-like cells • beat spontaneously and synchronously • teratomas after transplantation because of the unlimited differentiation potential of ESCs - need for selection • ethical concerns, potential genetic instability, risk of immune rejection - the ESCORT study Transplantation of Human Embryonic Stem Cell-derived Progenitors in Severe Heart Failure (ESCORT) (NCT02057900) induced Pluripotent Stem Cells (iPSCs) • forced expression of OCT4, SOX2, KLF4, and c-MYC transcription factors reprogram terminally differentiated • cells - resemble embryonic stem cells • iPSCs can be derived from individual patients for autologous transplantation • risk of teratoma formation, the low efficiency of cardiogenic differentiation, high costs, and timeconsuming methods • diagnostic methods – phenotype analyses and on demand patient specific drugs testing Derivation of Human Induced Pluripotent Stem (iPS) Cells to Heritable Cardiac Arrhythmias (NCT02413450), “Blood Collection From Healthy Volunteers and Patients forthe Production of ClinicalGrade Induced Pluripotent StemCell (iPSC) Products (NCT02056613),” Direct reprogramming? • additional slide according to question :-) • M. Ieda, J.-D. Fu, P. Delgado-Olguin et al., “Direct reprogramming of fibroblasts into functional cardiomyocytes by defined factors,” Cell, vol. 142, no. 3, pp. 375–386, 2010. Medicine paradigm shift! Gillray J. Bloodletting 1804, World History Archive