Recommended

Discover how to overcome low affinity or poor TCR yields that are slowing you down in this upcoming webinar – register your details today
WEBINAR | Discover how advances can expand the possibilities for drug discovery, from target validation to preclinical development
Facing roadblocks in obesity drug discovery? Discover how integrated, validated strategies are helping teams accelerate development and reduce risk – register your details now
Unlock the science, strategy and real-world impact behind the next generation of precision therapies – access our new brand report now >>
Safety data is no longer just a regulatory checkbox – it’s a strategic advantage. Find out more in our upcoming webinar, register your details today
WEBINAR | Join top cancer researchers to explore advances transforming early discovery, from new targets and models to the therapies of tomorrow
news

Normal liver cells may have the potential to kill cancer cells

A new discovery that healthy liver tissue surrounding a tumour activates a defence mechanism that restrains tumour growth could inspire new therapeutic approaches that mobilise normal cells to kill cancer cells. 

It has been discovered that healthy liver tissue surrounding a tumour activates a defence mechanism that restrains tumour growth. Hyperactivation of this mechanism above levels normally present in the liver triggered the elimination of different types of liver tumours in mice. 

This discovery identifies a novel strategy to fight against liver cancer and could inspire new therapeutic approaches that mobilise normal cells to kill cancer cells. 

The discovery was part of a study led by Professor Georg Halder and conducted at the VIB-KU Leuven Center for Cancer Biology, Belgium.

 

Reserve your FREE place

 


Are low affinity or poor TCR yields slowing you down?

Explore how CHO expression of soluble TCRs and TCR affinity maturation workflows via phage, serving as essential building blocks for early-stage TCR-TCE candidate generation.

22 October 2025 | 16:00 PM BST | FREE Webinar

Join Jiansheng Wu, Ph.D. to explore two integrated strategies:

  • High-titer CHO-based expression of sTCRs (~100 mg/L), enabling scalable and high-throughput production
  • Optimized phage display affinity maturation, improving TCR binding by up to ~10,000-fold

Whether you’re starting a new TCR program or optimizing an existing platform, this session will offer actionable strategies to accelerate discovery and improve candidate quality.

Register Now – It’s Free!

 

The study showed that non-cancerous liver cells around liver tumours have the capacity to kill nearby tumour cells. When they experimentally activated this novel mechanism in mice, the mice survived significantly longer and had a drastically reduced tumour burden.

“While the study shows that this anti-tumour mechanism exists, how exactly activated liver cells cause the elimination of cancer cells is not known,” said Professor Halder, “but it is obviously a highly significant question that we are currently investigating.”

The scientists found that the genes YAP and TAZ were activated around tumours in the liver and that this was the driving force of the anti-tumour mechanism. This is surprising because YAP and TAZ are usually highly expressed in different human cancers where they drive tumour cell proliferation and survival. 

While this study showed that this anti-tumour mechanism can kill tumours and metastases in the liver, it is not yet known whether similar mechanisms can be activated in other organs. “Given the striking anti-tumour effect of YAP-activated liver cells on liver tumours, our discovery has the potential to provide ground-breaking insights into a novel strategy to fight,” explained Stephanie Castaldo, co-first-author.

However, while this finding identifies a completely new strategy to fight cancer in mice, this study is the first molecular characterisation of this novel anti-tumour mechanism which means that more research is needed to investigate how these findings can be applied to benefit cancer patients. 

The results of the study were published in Science.

Leave a Reply

Your email address will not be published. Required fields are marked *