TY - JOUR TI - Patient-Derived Midbrain Organoids to Explore the Molecular Basis of Parkinson's Disease AU - Galet, Benjamin AU - Cheval, Hélène AU - Ravassard, Philippe T2 - Frontiers in Neurology AB - Induced pluripotent stem cell-derived organoids offer an unprecedented access to complex human tissues that recapitulate features of architecture, composition and function of in vivo organs. In the context of Parkinson’s Disease (PD), human midbrain organoid (hMO) are of significant interest, as they generate dopaminergic neurons expressing markers of Substantia Nigra identity, which are the most vulnerable to degeneration. Combined with genome editing approaches, hMO may thus constitute a valuable tool to dissect the genetic makeup of PD by revealing the effects of risk variants on pathological mechanisms in a representative cellular environment. Furthermore, the flexibility of organoid co-culture approaches may also enable the study of neuroinflammatory processes and interactions with other brain regions that are also affected over the course of the disease. We here review existing protocols to generate hMO, how they have been used so far to model PD, address a few of the challenges inherent to organoid cultures, and discuss applicable strategies to dissect the molecular pathophysiology of the disease. Taken together, the research suggests that this technology represents a promising alternative to 2D in vitro models, which could significantly improve our understanding of PD and help accelerate therapeutic developments. DA - 2020/// PY - 2020 DO - 10.3389/fneur.2020.01005 DP - Frontiers VL - 11 J2 - Front. Neurol. LA - English SN - 1664-2295 UR - https://www.frontiersin.org/articles/10.3389/fneur.2020.01005/full Y2 - 2020/09/09/17:58:20 KW - Dopamine KW - Genetics KW - IPS (induced pluripotent stem) cell KW - Organoid KW - Parkinson ' s disease KW - midbrain ER -