Gut microbiome modulates response to anti–PD-1 immunotherapy in melanoma patients

Gopalakrishnan, Vancheswaran; Spencer, Christine N.; Nezi, Luigi; Reuben, Alexandre; Andrews, Miles C.; Karpinets, Tatiana V.; Prieto, Peter A.; Vicente, Diego; Hoffman, Kristi L.; Wei, Spencer C.; Cogdill, Alexandria P.; Zhao, Li; Hudgens, Courtney W.; Hutchinson, Diane S.; Manzo, Teresa; Macedo, Mariana Petaccia de; Cotechini, Tiziana; Kumar, Tapsi; Chen, W. S.; Reddy, Sangeetha M.; Szczepaniak-Sloane, Robert; Galloway-Peña, Jessica; Jiang, Hong; Chen, P. L.; Shpall, Elizabeth J.; Rezvani, Katayoun; Alousi, Amin M.; Chemaly, Roy F.; Shelburne, Samuel A.; Vence, Luis M.; Okhuysen, Pablo C.; Jensen, Vanessa; Swennes, Alton G.; McAllister, Florencia; Sanchez, Erick Marcelo Riquelme; Zhang, Y.; Zitvogel, Laurence; Pons, Nicolas; Austin-Breneman, Jacob L.; Haydu, Lauren E.; Burton, Elizabeth M.; Gardner, Julie M.; Sirmans, Elizabeth; Hu, Jiemiao; Lazar, Alexander J.; Tsujikawa, Takahiro; Diab, Adi; Tawbi, Hussein A.; Glitza, Isabella C.; Hwu, Wen Jen; Patel, Sapna; Woodman, Scott E.; Amaria, Rodabe N.; Davies, Michael A.; Gershenwald, Jeffrey E.; Hwu, Patrick; Lee, J. E.; Zhang, J.; Coussens, Lisa M.; Cooper, Zachary A.; Futreal, P. Andrew; Daniel, Carrie R.; Ajami, Nadim J.; Petrosino, Joseph F.; Sharma, Pradeep; Allison, James P.; Jenq, Robert R.; Wargo, Jennifer A.

doi:10.1126/science.aan4236

Cited by 3,180 publications

(2,879 citation statements)

References 79 publications

Supporting

Mentioning

2,780

Contrasting

Unclassified

Order By: Relevance

“…Wargo's group (MD Anderson Cancer Center, Houston, Texas, USA) explored the role of oral and gut microbiome in anti-PD1-treated melanoma patients by 16S rRNA gene sequencing [8]. The oral microbiome did not reveal differences between R and NR patients.…”

mentioning

confidence: 99%

Anti-PD1 in the wonder-gut-land

Vétizou

Trinchieri

2018

Cell Res

View full text Add to dashboard Cite

mentioning

confidence: 99%

Anti-PD1 in the wonder-gut-land

Vétizou

Trinchieri

2018

Cell Res

View full text Add to dashboard Cite

“…Through comparing fecal samples from 112 MM patients taking anti-PD-1 Ab therapies, Wargo and colleagues found that responders had a significantly higher abundance of commensals of the Clostridales order and the Bacteroidales order, belonging to the Firmicutes phylum and Bacteroidetes phylum respectively. 38 Even though there was a clear difference in the cancer types studied between this publication and the 2017 publication by Zitvogel and colleagues, there were key similarities between the microbial profiles associated with response. Therefore, the species of commensal bacteria found essential for response may have little to do with the type of cancer which anti-PD-1 Ab targets.…”

mentioning

confidence: 83%

“…35 , 36 A study by Herold and colleagues in December 2017 found systemic immune activation in humanized mice models given anti-CD3 mAb in combination with antibiotics, shown through elevated numbers of effector T-cells and IFN-γ, decreased production of IL-10, and the presence of anti-nuclear antibodies. 35 While there are other investigations demonstrating that gut dysbiosis, or a microbial imbalance or modification in the host gut, may counteract the effects of both immunosuppressive 35 and immunostimulatory drugs, 3 , 23 , 27 , 37 , 38 it may be that microbiota have a more potent or direct interaction with the immune checkpoint drugs rather than the immunomodulatory cells involved per se. All in all, these apparent contradictions reinforce that the function and mechanisms by which commensal bacteria communicate with the immune system are poorly understood and remain a fascinating challenge for prospective researchers.…”

mentioning

confidence: 99%

“…Comparable to what was discovered in their 2015 publication, the authors measured an increase in stool richness, at the metagenomics species level, of the NSCLC and RCC patients after two months since their first injection of anti-PD-1 Ab. Moreover, a response to anti-PD-1 Ab has been shown to be associated with significantly higher alpha diversity of gut microbiota 38 and interestingly, increased levels of CTLA-4 hi PD-1 hi CD8+ T-cells. 25 Corresponding proportions are thus suggestive of a situational positive feedback mechanism where TILs or other systemic lymphocytes signal the proliferation of certain bacteria or possibly enrich the ecosystem in the gut to establish a more tolerable living environment for the gut microbiome.…”

mentioning

confidence: 99%

See 1 more Smart Citation

The gut microbiota and immune checkpoint inhibitors

Humphries

Daud

2018

Human Vaccines & Immunotherapeutics

View full text Add to dashboard Cite

Although immunotherapy has been remarkably effective across multiple cancer types, there continues to be a significant number of non-responding patients. A possible factor proposed to influence the efficacy of immunotherapies is the gut microbiome. We discuss the results and implications of recent research on the relationship between the gut microbiome, our immune systems, and immune checkpoint inhibitor therapies including anti-CTLA-4 Ab and anti-PD-1 Ab. While the investigations all exhibit interesting results and conclusions, we find little congruence in the specific bacteria that were found favorable for antitumor responses. It is unclear whether the inconsistencies are due to differential approaches in study design (pre-clinical or clinical subjects, anti-CTLA-4 Ab or anti-PD-1 Ab), experimental methods and measurements (metagenomics sequencing and clustering variations) or subject population dynamics (differential cancer types and baseline characteristics). Moreover, we note studies regarding particular bacterial commensals and autoimmune diseases, which challenge findings from these investigations. We conclude that with the current research, clinical investigators can appreciate the critical role of gut microbiota in mediating immunostimulant response. However, prospective research exploring the biochemical mechanisms which commensal bacteria communicate with each other and the immune system is imperative to understand how they can be adjusted properly for higher immunotherapy response.

show abstract

“…Recent reports suggested that host microbiome and tumor and stromal genomic profiles may be related with response to immune checkpoint blockade [9,10] . The diversity and abundance of specific bacterial species in the oral and fecal microbiome enhanced systemic and antitumor immunity [43,44] . For example, in the patients with advanced tumor who received immunotherapy, the use of antibiotics caused poor prognosis.…”

Section: Future Prospect Of Immunotherapymentioning

confidence: 99%

Management of metastatic esophagogastric junction adenocarcinoma

Toihata¹,

Imamura²,

Watanabe³

et al. 2018

JCMT

View full text Add to dashboard Cite

The prognosis of metastatic disease of esophagogastric junction adenocarcinoma remains poor, despite using a variety of regimens using cytotoxic agents. Recent understanding of molecular characteristic and tumor microenvironment of this cancer is currently instigating new therapeutic options. In this review, we summarized previous evidences of cytotoxic agents widely used worldwide, and updated recent developments of molecular targeted drugs, and immune checkpoint inhibitors.

show abstract

Gut microbiome modulates response to anti–PD-1 immunotherapy in melanoma patients

Cited by 3,180 publications

References 79 publications

Anti-PD1 in the wonder-gut-land

Anti-PD1 in the wonder-gut-land

The gut microbiota and immune checkpoint inhibitors

Management of metastatic esophagogastric junction adenocarcinoma

Contact Info

Product

Resources

About