Highlights:
A new class of immunotherapeutic agents that are more effective at harnessing the power of the immune system to fight cancer has been invented by a research team at Johns Hopkins University School of Medicine.
Their approach results in significant inhibition of tumor growth, even against cancers which do not respond to existing immunotherapies used in the clinic. The team worked in collaboration with Insilico Medicine, a Baltimore-based leader in artificial intelligence for drug discovery.- A new class of immunotherapeutic agents has been invented.
- These agents are called Y-traps as they trap Y-shaped antibodies.
- Y-traps can unleash agents of the immune system to treat cancers that have become resistant to other treatments.
Radiotherapy - Background
A detailed account of radiation, its mode of action, side effects and dosage in the treatment of cancer.
A detailed account of radiation, its mode of action, side effects and dosage in the treatment of cancer.
‘A new class of immunotherapeutic agents called “Y-traps” has been invented by a research team at Johns Hopkins University School of Medicine. These agents can trap and unleash antibodies (agents of the immune system) that are shaped like a ‘Y’ to fight cancer.’
Tweet it Now
Virtually all cancers, including the most common cancers, from lung, breast, and colon cancers to melanomas and lymphomas, evolve to defeat immune surveillance by amplifying natural mechanisms of immune suppression. Current clinical immunotherapy relies on using antibodies to disable specific molecules, such as CTLA-4 and PD-1/PD-L1, which function as natural brakes to suppress immune cells. Antibodies that counteract these checkpoints can unleash the immune system to attack cancer cells. While they produce lasting responses in some cases, these therapies are not effective in the vast majority of patients.The research team finds that a major reason for the failure of immune checkpoint inhibitors is the ability of tumors to produce transforming growth factor-B (TGFB). TGFB plays a key role in immune regulation and development of immunosuppressive regulatory T cells (Tregs). Using Insilico Medicine software, the team found that TGFB pathway activation in various cancers is highly correlated with FOXP3, the signature of Tregs. Tumors are frequently infiltrated by Tregs, and this is strongly correlated with poor outcome in multiple cancer types.
Y-traps - the new class of immunotherapeutic agents
To address this challenge, the team invented Y-traps, a new class of bifunctional immunotherapeutic agents consisting of a targeting antibody (shaped like a "Y"), fused to a "trap" that disables an immunosuppressive molecule. To sequester TGFB, they engineered a trap based on the natural receptor to TGFB. They created two different types of Y-traps: one consisting of a CTLA-4 antibody fused to a TGFB trap, and another consisting of a PD-L1 antibody fused to a TGFB trap.
Soft Tissue Sarcoma - Types, Causes, Symptoms, Diagnosis, Treatment & Prevention
Soft tissue sarcoma is a rare cancer of connective tissue that can affect soft tissues such as fat, muscle, nerves and blood vessels of any body part.
Soft tissue sarcoma is a rare cancer of connective tissue that can affect soft tissues such as fat, muscle, nerves and blood vessels of any body part.
While the clinically-used CTLA-4 antibody, ipilimumab, could not decrease Tregs in these tumors, the CTLA4-targeted Y-trap was strikingly effective at reducing Tregs and activating antitumor immunity. Most significantly, the Y-trap was remarkably effective at inhibiting the growth and spread of tumors that were unresponsive to treatment with ipilimumab and pembrolizumab, a PD-1 antibody used in the clinic.
Advertisement
Triple-Negative Breast Cancer - Causes, Symptoms, Diagnosis, Treatment, Prevention & Prognosis
Triple-negative breast cancers are ER negative, PR negative, and lack overexpression of HER-2. They are difficult to treat and are very aggressive.
Triple-negative breast cancers are ER negative, PR negative, and lack overexpression of HER-2. They are difficult to treat and are very aggressive.
What the Y-traps offer to oncology
Bedi and colleagues demonstrated that the PD-L1 targeted Y-Trap is significantly more effective in inhibiting tumor growth compared to clinically-used PD-L1 antibodies, atezolizumab and avelumab. Moreover, the PD-L1-targeted Y-trap was able to curtail the growth of tumors that do not respond to PD-L1 or PD-1 antibodies.
Advertisement
Why is Health Screening in Women between 40 and 60 years of age important?
Health screening in women between 40 and 60 years helps to diagnose health issues in the early stages when they can be controlled. This ensures a more comfortable old age.
Health screening in women between 40 and 60 years helps to diagnose health issues in the early stages when they can be controlled. This ensures a more comfortable old age.
"Since these mechanisms of immune dysfunction are shared across many types of cancer, the Y-trap approach could have broad impact for improving cancer immunotherapy," says Bedi.
"This approach appears to be an innovative strategy, and an exciting technical accomplishment to target multiple suppressive mechanisms in the tumor microenvironment," says Robert Ferris, MD, Ph.D, professor of oncology at the University of Pittsburgh, who was not connected with the study. "I look forward to seeing its translation into the clinic."
Bedi envisions using Y-traps not only for treatment of advanced, metastatic disease, but also in the neoadjuvant setting to elicit a vaccine effect, that is, giving them to patients before surgery to prevent recurrence of the disease.
References:
- Rajani Ravi, Kimberly A. Noonan et al. Bifunctional Immune Checkpoint-targeted Antibody-ligand Traps that Simultaneously Disable TGFβ Enhance The Efficacy of cancer Immunotherapy, Nature Communications doi:10.1038/s41467-017-02696-6
Source-Eurekalert
