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This book summarizes early pioneering achievements in the field of
human neural stem cell (hNSC) research and combines them with the
latest advances in stem cell technology, including reprogramming
and gene editing. The powerful potential of hNSC to generate and
repair the developing and adult CNS has been confirmed by numerous
experimental in vitro and in vivo studies. The book presents
methods for hNSC derivation and discusses the mechanisms underlying
NSC in vitro fate decisions and their in vivo therapeutic mode of
action. The long-standing dogma that the human central nervous
system (CNS) lacks the ability to regenerate was refuted at the end
of the 20th century, when evidence of the presence of neurogenic
zones in the adult human brain was found. These neurogenic zones
are home to human neural stem cells (hNSCs), which are capable of
self-renewing and differentiating into neurons, astrocytes and
oligodendrocytes. NSCs isolated from human CNS have a number of
clinical advantages, especially the innate potential to
differentiate into functional neural cells. Nevertheless, their
full clinical exploitation has been hindered by limited access to
the tissue and low expansion potential. The search for an
alternative to CNS sources of autologous, therapeutically competent
hNSCs was the driving force for the many studies proving the in
vitro plasticity of different somatic stem cells to generate NSCs
and their functional progeny. Now the era of induced pluripotent
stem cells has opened entirely new opportunities to achieve
research and therapeutic goals with the aid of hNSCs.
This book summarizes early pioneering achievements in the field of
human neural stem cell (hNSC) research and combines them with the
latest advances in stem cell technology, including reprogramming
and gene editing. The powerful potential of hNSC to generate and
repair the developing and adult CNS has been confirmed by numerous
experimental in vitro and in vivo studies. The book presents
methods for hNSC derivation and discusses the mechanisms underlying
NSC in vitro fate decisions and their in vivo therapeutic mode of
action. The long-standing dogma that the human central nervous
system (CNS) lacks the ability to regenerate was refuted at the end
of the 20th century, when evidence of the presence of neurogenic
zones in the adult human brain was found. These neurogenic zones
are home to human neural stem cells (hNSCs), which are capable of
self-renewing and differentiating into neurons, astrocytes and
oligodendrocytes. NSCs isolated from human CNS have a number of
clinical advantages, especially the innate potential to
differentiate into functional neural cells. Nevertheless, their
full clinical exploitation has been hindered by limited access to
the tissue and low expansion potential. The search for an
alternative to CNS sources of autologous, therapeutically competent
hNSCs was the driving force for the many studies proving the in
vitro plasticity of different somatic stem cells to generate NSCs
and their functional progeny. Now the era of induced pluripotent
stem cells has opened entirely new opportunities to achieve
research and therapeutic goals with the aid of hNSCs.
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