In vivo monitoring of remnant undifferentiated neural cells following human induced pluripotent stem cell-derived neural stem/progenitor cells transplantation.
Yuji TanimotoTomoteru YamasakiNarihito NagoshiYuichiro NishiyamaSatoshi NoriSoraya NishimuraTsuyoshi IidaMasahiro OzakiOsahiko TsujiBin JiIchio AokiMasahiro JinzakiMorio MatsumotoYasuhisa FujibayashiMing-Rong ZhangMasaya NakamuraHideyuki OkanoPublished in: Stem cells translational medicine (2020)
Transplantation of human-induced pluripotent stem cell-derived neural stem/progenitor cells (hiPSC-NS/PCs) is a promising treatment for a variety of neuropathological conditions. Although previous reports have indicated the effectiveness of hiPSC-NS/PCs transplantation into the injured spinal cord of rodents and nonhuman primates, long-term observation of hiPSC-NS/PCs post-transplantation suggested some "unsafe" differentiation-resistant properties, resulting in disordered overgrowth. These findings suggest that, even if "safe" NS/PCs are transplanted into the human central nervous system (CNS), the dynamics of cellular differentiation of stem cells should be noninvasively tracked to ensure safety. Positron emission tomography (PET) provides molecular-functional information and helps to detect specific disease conditions. The current study was conducted to visualize Nestin (an NS/PC marker)-positive undifferentiated neural cells in the CNS of immune-deficient (nonobese diabetic-severe combined immune-deficient) mice after hiPSC-NS/PCs transplantation with PET, using 18 kDa translocator protein (TSPO) ligands as labels. TSPO was recently found to be expressed in rodent NS/PCs, and its expression decreased with the progression of neuronal differentiation. We hypothesized that TSPO would also be present in hiPSC-NS/PCs and expressed strongly in residual immature neural cells after transplantation. The results showed high levels of TSPO expression in immature hiPSC-NS/PCs-derived cells, and decreased TSPO expression as neural differentiation progressed in vitro. Furthermore, PET with [18 F] FEDAC (a TSPO radioligand) was able to visualize the remnant undifferentiated hiPSC-NS/PCs-derived cells consisting of TSPO and Nestin+ cells in vivo. These findings suggest that PET with [18 F] FEDAC could play a key role in the safe clinical application of CNS repair in regenerative medicine.
Keyphrases
- induced apoptosis
- pet imaging
- positron emission tomography
- dengue virus
- cell cycle arrest
- computed tomography
- stem cells
- spinal cord
- pet ct
- randomized controlled trial
- endoplasmic reticulum stress
- type diabetes
- signaling pathway
- zika virus
- spinal cord injury
- early onset
- small molecule
- neuropathic pain
- combination therapy
- aedes aegypti
- protein protein
- subarachnoid hemorrhage
- pi k akt