The team also saw that regions with bacteria were more likely to be necrotic, with fewer dividing cells. It might sound like bad news for the tumor, but other research has shown that the tumor cells that spread and metastasize through the body often break away from necrotic areas. Cells can’t migrate while they’re rapidly dividing, so conditions that encourage cells to stop growing and start moving are conditions that can promote metastasis.
It looked like F. nucleatum could be encouraging tumor progression and immune evasion, but the data was correlative and couldn’t rule out the possibility that the microbes are just attracted to necrotic, already-immunosuppressed areas. To examine how bacteria may influence tumors, the team used tumor spheroids, which are tumor cells grown in 3D clusters in the laboratory.
To assess whether bacteria may promote an immunosuppressive environment, the scientists grew colorectal cancer spheroids with immune cells called neutrophils. Neutrophils crawled around and through tumor spheroids without bacteria. But when the investigators added F. nucleatum to the spheroids, they saw that neutrophils stopped moving and clustered within spheroids.
“The neutrophils migrated inside the spheroid and appeared trapped,” Galeano Niño said. “It supported what we saw in the patient spatial data: That there were neutrophils in the regions colonized by bacteria. That's interesting because neutrophils negatively impact T-cell activity. This could perhaps explain what we’re seeing with the T-cell exclusion in those regions colonized by bacteria.”
The team also saw that tumor cells in the spheroids moved differently when bacteria were present. In spheroids without bacteria, the tumor cells moved en masse, which helped the spheroids grow larger, but didn’t help them release single cells capable of seeding new metastases.
“When bacteria were present, the cancer epithelial cells migrated as single cells — and they brought bacteria with them,” Bullman said.
The finding is in line with Bullman’s previous work, in which she had shown that F. nucleatum often travels with colorectal cancer metastases.
But how exactly are bacteria interacting with and influencing cells? To learn more, the team adapted single-cell transcriptome sequencing technologies for bacteria, developing an approach they called INVADEseq (Invasion Adhesion Directed Expression sequencing).
Using INVADEseq, the team saw that tumor cells infected with bacteria ramped up genes associated with cancer progression and metastasis. In oral tumor samples, the investigators saw that bacteria preferentially infected cancer epithelial cells and specific immune cell types within patients’ tumors. Infected tumor cells were more likely to have turned on genes involved in responding to DNA damage, which is a hallmark of cancer.
“The functional work supports [the idea] that the bacteria have a direct role in shaping these micro-niche regions,” Bullman said.
Tumor microbiome influences drug efficacy
If bacteria are promoting tumor progression, treating bacteria seems like an obvious way of also treating the tumor. Bullman’s previous study supported this idea: when she treated mice engrafted with human tumor tissue with antibiotics, this slowed the growth of colorectal cancers positive for F. nucleatum.
“This raises the possibility of targeting specific members of the microbiota for patient cancer treatment,” Bullman said.
But that proof-of-principle work relied on metronidazole, a drug that kills off a wide range of bacteria, even those that benefit us.
“You don’t want to knock out all the beneficial microbes within a patients microbiota — this needs to be very targeted,” she said. “So, we designed a small-molecule screen of over 1,800 compounds to try and identify narrow-spectrum inhibitors of F. nucleatum.”
Surprisingly, about 15% of the antimicrobials that meet this criterion were also chemotherapeutics — including 5-fluorouracil, or 5-FU, which is already routinely used to treat colorectal cancer.
The researchers found that F. nucleatum is extremely sensitive to 5-FU.
“That was really surprising to us,” Bullman said. “It raises the possibility that part of 5-FU’s treatment efficacy could be due to its antimicrobial activity.”
But for many patients, 5-FU treatment doesn’t prevent tumor growth. Could the tumor microbiota be contributing to this? When the team tested 5-FU against other bacterial strains taken from colorectal cancer samples, they saw that several, including a strain of E. coli, resisted its inhibitory effects. Growing this strain of E. coli with F. nucleatum protected F. nucleatum from 5-FU. (Another tumor-derived bacterial species they tested was unable to rescue F. nucleatum from the drug’s effects.)
The researchers then found that E. coli protected colorectal cancer cells from 5-FU as well. The E. coli appeared to have a way of metabolizing the drug and minimizing its exposure to cancer cells or other bacteria.
“The findings show that intra-tumoral microbes are not innocent bystanders during disease progression, and suggest that the microbiota should be taken into consideration when thinking about optimal cancer treatments,” Johnston said.
Avenues to explore new treatments
The work further supports the idea that a tumor’s microbiota is an under-appreciated vulnerability and a potential treatment target. It appears that for some cancers, bacteria are important contributors to almost every step of tumor development and can even help shield it against treatment. Therapeutics that effectively modulate a tumor’s microbiota could help slow its growth as well as stave off metastasis or hobble cancer cells that have already spread.
The detailed analysis of bacterial species in both colorectal and oral tumors may also point to good oral health as an important way to help reduce cancer risk.
In addition to its cancer associations, F. nucleatum is linked to periodontal disease — and it wasn’t the only oral bacteria the team saw inside tumor cells from patients. Another oral bacterial genus linked to gum disease, called Treponema, also made its way inside tumor cells. These bacteria have also been linked to oral cancer, though the associations are less strong than F. nucleatum’s with colorectal cancer.
“There is a trend emerging of microbes that are traditionally associated with oral inflammatory disease being found in association with extra-oral and gastrointestinal cancers — which highlights the oral cavity as a breeding ground for pathogenic onco-microbes,” Johnston said.
In addition to allowing pathogens to spread to new areas of the body, it is possible that inflammation in the mouth, in the form of periodontal or endodontic disease, could be selecting for and encouraging the outgrowth of bacteria that are more specialized for growth in adverse conditions and capable of evading immune attack, he said.
Whether other tumors also harbor distinct bacterial micro-niches, and how these regions differ from non-colonized regions, are further questions Bullman and Johnston hope to answer. The team is exploring whether they can make tumors more responsive to immunotherapy or chemotherapy by manipulating their microbiomes. The first challenge will be developing strategies that are able to reach bacteria inside tumors. Further down the line, they hope to capitalize on the underlying biology of these tumor-homing microbes to develop novel therapeutic interventions, a strategy dubbed “bugs as drugs.”
By showing that microbes cluster in hard-to-reach areas of tumors, the same areas that are recalcitrant to current therapeutic regimens, the work clarified some hurdles that the team need to overcome in the development of new therapeutics.
“This holistic approach to assessing the tumor microenvironment, which is a multi-species ecosystem, will advance our understanding of cancer biology, and I believe will reveal new therapeutic vulnerabilities in cancer,” Bullman said.
This work was supported by the National Institutes of Health, the National Institute of Dental and Craniofacial Research, the National Cancer Institute, an Irvington Postdoctoral Fellowship from the Cancer Research Institute and a Washington Research Foundation Fellowship.