Proteolysis-targeting
chimeras (PROTACs) is a fast-growing technology
providing many strengths over inhibition of protein activity directly
and is attracting increasing interest in new drug discovery and development.
However, efficiently identifying potent and drug-like degraders is
still challenging in the development of PROTACs. Complementary to
traditional PROTACs, several emerging types of PROTACs, such as homobivalent
PROTACs based on two E3 ligases (e.g., CRBN, VHL, MDM2, TRIM24), chemical-
or biological-based trivalent/multitargeted PROTACs, and covalent
PROTACs, are rising for targeted protein degradation. These new types
of PROTACs have several advantages over the traditional PROTACs including
high selectivity, low toxicity, better therapeutic effects, and so
on. In this perspective, we will summarize the latest development
of representative PROTACs focusing on research mainly in past 10 years
and discuss their advantages and disadvantages. Moreover, the outlook
and perspectives on the associated challenges and future directions
will be provided.