Table 2.
Pros and cons of different strategies to open the BBB
| Strategies | Methods | Pros | Cons | Ref. | |
|---|---|---|---|---|---|
| Transient disruption of BBB tight junctions | Chemical methods: | Osmotic agents (mannitol) |
Clinic approved. Rapid onset of action (within 5 to 10 min after administration) which results in opening the BBB to a wide range of substances |
Short half‐life and side effects, such as inducing seizures and increasing intracranial pressure | [139, 140, 141, 142] |
| Angiogenic molecules (VEGFA) | Approved in the clinic | Non‐specific opening of the BBB, which may cause side effects | [ 35 ] | ||
| S1P | Broad effects, including regulation of brain endothelial cell junction, transcytosis, and efflux transporter activity | Dose‐sensitive | [143, 144] | ||
| S1PR1 modulator: Fingolimod | Approved in the clinic | Size‐selective opening of the BBB, Controversial effects on BBB integrity | [97, 145] | ||
| Autoantibodies (GRP78) | Opening of the BBB to macromolecules | Inflammation‐induced BBB breakdown may be harmful | |||
| Physical method: | MR‐FUS | Highly efficient, enables focus on targeted region, promising results in multiple clinical trials | Sensitive to ultrasound intensity, may cause side effects such as chronic inflammation | [33, 146, 147, 148] | |
| Overcoming efflux transporters | Inhibitors of P‐gp and BCRP1 | Some inhibitors are approved in the clinic | Mixed results in clinical studies. Potential side effects as P‐gp and BCRP1 are critical for metabolism and excretion of cytotoxic agents from the brain. | [132, 134, 149, 150] | |