(A) Expansion of MuSCs isolated from enzymatically digested skeletal muscles under standard culturing conditions on plastic dishes (upper path) selects for myoblasts with poor regenerative and engraftment capability. Two main strategies have been proposed to preserve the in vivo regenerative potential of MuSCs during in vitro culturing and resulted in productive engraftment in preclinical studies. One strategy (middle path) consists of the manipulation of artificial culturing substrates with bioengineering techniques to mimic the niche in which MuSCs reside and stimulate quiescence. The second strategy (lower path) consists of the adoption of culturing conditions favoring the expansion of myogenic progenitors with preserved regenerative potential. (B) Expansion of myogenic progenitors with preserved regenerative potential can be achieved through the addition to the culture medium of factors able to modulate the activity of fundamental signaling pathways, such as the Notch, JAK/STAT, oncostatin M (Osm), and p38 MAPK signaling pathways (34, 138–140, 142); Setd7-dependent epigenetic modifications (143); eIF2α-dependent translational control (141); or the genetic alteration of regulators of myogenic lineage progression and proliferation.