Researchers use “hallmarks of cancer” to understand tumour growth

Under this new light, tumour architecture emerges as a valuable source of information to understand tumour dynamics and predict its sensitivity to anticancer drugs. 

The output of the collaboration was recently published at the journal Cell Reports. 

“What is a tumour?” This is the fundamental question to answer if we want to treat cancer effectively. Our vision of cancer and tumours has been evolving with time, from the simplistic bunch of all-similar malignant cells to a more sophisticated, heterogeneous and hierarchical cellular structure, composed of many different cell types. Recently, a new paradigm has emerged: the hallmarks of cancer.

Click to enlarge: Quantifying the activity of cancer hallmarks across space: (A) Overview of the spatial transcriptomics cohort, showing the number of samples for each tumor type studied. (B) Workflow to build cancer hallmark signatures. (C) Comparison between H&E images (top) and the hallmark’s activity (bottom) in five of the studied cancer types. (D) Ridge plot showing the spatial autocorrelation distribution for each of the 13 cancer hallmarks across 63 samples. Higher values indicate non-random clustering, while lower values suggest random distribution within the tissue.

Image source: Sibai M, Cervilla S, Grases D et al., Cell Reports 2025 (CC BY-NC-ND 4.0)

The hallmarks of cancer are features that, when unlocked in a cell, put it in the road to malignant transformation, to express it in simple words. So far, there are 13 hallmarks, and each is defined by the expression of a set of genetic pathways, that can be identified in the lab by using genomics tools. Previous research showed that not all cells express all the hallmarks in a tumour so, how is hallmarks expression organised? And, most importantly, does this have any clinical implications? 

To answer these questions, Dr. Eduard Porta, principal researcher of the Cancer Immunogenomic laboratory at the Josep Carreras Leukaemia Research Institute (IJC) and researcher of the Computational Biology group at the Barcelona Supercomputing Center – Centro Nacional de Supercomputación (BSC-CNS), led a team of renowned scientists, including Dr. Esteller (IJC), Dr. Barretina (IGTP), Dr. Real (CNIO) and Dr. Bailey (Simmons Center for Cancer Research, USA). The output shows the thorough analysis of 63 tumour samples from 10 common malignancies, including breast, lung, prostate and colorectal cancer. Dr. Mustafa Sibai signs the article as lead author. 

In the research, they used a totally new approach and focused on the identification of the different functionalities of each cell into the tumour, according to its hallmark’s expression instead of cell-type. In this way, they could see how malignant cells specialised in growing the tumour, while non-cancer cells surrounding it – called the tumour microenvironment – contributed with the suppression of the immune system or preventing the efficient delivery of anticancer drugs, for example.

Also, the different hallmarks were found to be expressed in cells located in specific areas within the tumour, a feature seen also in tissue and organ development. On this regard, the position of different hallmarks was found to be not random but followed a pattern that could be seen across all the tumours in the study and, probably, in many other cancer types. 

Furthermore, it seemed that hallmarks may influence each other, and the position of ones can be predicted by the presence of others, using machine learning algorithms. This would be a disruptive vision on tumour evolution, moving from a selection-based paradigm to an ecological perspective where function, expressed in terms of hallmarks, could be the golden rule. “Our findings show that tumors aren’t just random collections of cancer cells. They are highly organized ecosystems where different regions perform specific roles," said Dr. Eduard Porta-Pardo, senior author of the study, and adds that "understanding these spatial patterns helps us identify which tumors are more likely to respond to certain treatments." 

While this debate might look like highly academic, the results of the research goes way beyond answering fundamental questions and have a real impact on actual cancer patients. The team checked whether hallmark expression patterns impacted the clinical management of 33 bladder cancer patients in the DUTRENEO trial and found that differences in the hallmarks could explain the success or failure of adjuvant therapy, opening the door to a new therapeutical approach in the future. “By identifying hallmark ‘hotspots’ linked to drug resistance, we can improve how therapies are tailored to individual patients”, says Dr. Sibai and, as an actual example, Dr. Manel Esteller, co-senior author of the research, explains that “for immune checkpoint inhibitors to be effective, it is not sufficient for a cancer cell to merely display markers of response. The surrounding cells must also create a supportive environment for the immunotherapy to work.” 

It feels like researchers are really getting closer and closer to answering the fundamental question of “what is a tumour?” and, while doing so, new advances appear to help fight against cancer more effectively. 

Source: Josep Carreras Leukaemia Research Institute

30.01.2025

• cancer (940)
• research (3252)
• tumour (345)