Alkylresorcinols as a New Type of Gut Microbiota Regulators Influencing Immune Therapy Efficiency in Lung Cancer Treatment

Author:

Shestopalov Aleksandr V.123ORCID,Kit Oleg I.4,Zabolotneva Anastasia A.1ORCID,Zlatnik Elena Y.4,Maksimov Aleksey Yu4,Novikova Inna A.4,Sagakyants Alexander B.4,Timofeeva Sofya V.4,Goncharova Anna S.4,Galina Anastasia V.4,Appolonova Svetlana A.5ORCID,Markin Pavel A.5,Makarov Valentin V.6,Yudin Sergey M.6,Keskinov Anton A.6,Roumiantsev Sergei A.12ORCID,Meshkov Oleg I.6

Affiliation:

1. N. I. Pirogov Russian National Research Medical University, 117997, 1 Ostrovitianov Str., Moscow, Russia

2. Center for Digital and Translational Biomedicine “Center for Molecular Health”, 117218, 32 Nakhimovsky Prospekt, Moscow, Russia

3. Rogachev National Medical Research Center of Pediatric Hematology, Oncology, and Immunology, 117997, 1 Samory Mashela Str., Moscow, Russia

4. National Medical Research Centre for Oncology, 344019, 14 Line 63, Rostov-on-Don, Russia

5. Sechenov First Moscow State Medical University, 119991, 2-4 Bolshaya Pirogovskaya Str., Moscow, Russia

6. Center for Strategic Planning and Management of Medical and Biological Health Risks of FMBA of Russia, 119121, Pogodinskya Str., h.10, b.1, Moscow, Russia

Abstract

Background. Alkylresorcinols (ARs) are polyphenolic compounds of microbial origin with a wide spectrum of biological activities and are potentially involved in host immune functioning. The present study is aimed at evaluating alterations in AR content in blood serum and faeces from healthy donors and patients with lung cancer in connection with response to immune checkpoint inhibitor (ICI) therapy to estimate the regulatory potential of AR. Methods. Quantitative analysis of AR levels, as well as other microbial metabolites in blood serum and faeces, was performed using gas chromatography with mass spectrometric detection; estimation of lymphocyte subsets was performed by flow cytometry; faecal microbiota transplantation (FMT) from lung cancer patients after ICI therapy to germ-free mice was performed to explore whether the intestinal microbiota could produce AR molecules. Results. AR concentrations in both faeces and serum differ dramatically between healthy and lung cancer donors. The significant increase in AR concentrations in mouse faeces after FMT points to the microbial origin of ARs. For several ARs, there were strong positive and negative correlations in both faeces and serum with immune cells and these interrelationships differed between the therapy-responsive and nonresponsive groups. Conclusions. The content of ARs may influence the response to ICI therapy in lung cancer patients. ARs may be considered regulatory molecules that determine the functioning of antitumor immunity.

Funder

Center for Strategic Planning and Management of Medical and Biological Health Risks of FMBA of Russia

Publisher

Hindawi Limited

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