The success of early CAR-T cell therapies was partly luck. Future therapies face a high bar, as an ideal target must meet three criteria: 1) be abundant on cancer cells, 2) be indispensable for the cancer's survival, and 3) be dispensable for the patient's healthy tissues to avoid lethal toxicity.

The field of sarcoma treatment has seen rapid progress by shifting from "one-size-fits-all" clinical trials to studies focused on specific histological subtypes. This targeted approach led to nearly 10 FDA approvals since 2019, revolutionizing care for these rare cancers.

T-cell receptor (TCR) therapies offer a significant advantage over monoclonal antibodies by targeting intracellular proteins. They recognize peptides presented on the cell surface, effectively unlocking 90% of the proteome and requiring far fewer target molecules (5-10 copies vs. 1000+) to kill a cancer cell.

An innovative strategy for solid tumors involves using bispecific T-cell engagers to target the tumor stroma—the protective fibrotic tissue surrounding the tumor. This novel approach aims to first eliminate this physical barrier, making the cancer cells themselves more vulnerable to subsequent immune attack.

Developing CAR T-cell therapies for solid tumors is difficult because many tumor-associated antigens are also expressed on normal tissues. This creates a significant risk of "on-target, off-tumor" effects, causing severe toxicity. Mitigating this risk, for instance with engineered "kill switches," is as crucial as preserving the therapy's efficacy.

To increase safety and efficacy, next-generation CAR-T therapies use "logic-gated" designs. These constructs only activate when they detect the co-expression of multiple antigens—a signature unique to tumor cells—thereby avoiding off-target toxicity on healthy tissues that may express only one of the antigens.

Instead of focusing solely on T-cells, Create's platform first targets myeloid cells, which constitute up to 60% of some solid tumors. Programming these cells transforms the tumor microenvironment, enabling a 5-10x influx of CD8 T-cells. This overcomes a key barrier for T-cell therapies in solid tumors.

Companies like VIR are making progress with masked T-cell engagers that limit systemic toxicity like cytokine release syndrome (CRS). This approach, which concentrates efficacy at the tumor site, could be the key to unlocking the broad potential of T-cell engagers beyond hematologic malignancies into the much larger solid tumor market.

Many promising solid tumor antigens (e.g., PSMA, HER2) are also on normal tissues, making them too toxic for T-cell engagers. By using masks that are cleaved only in the tumor microenvironment, these "dirty" targets become viable, dramatically expanding the therapeutic landscape for solid cancers.