ARACHIDONIC ACID ENHANCES MITOPHAGY AND DECREASES INFLAMMATORY RESPONSE IN PRIMARY MACROPHAGES



Cite item

Full Text

Abstract

Abstract

Macrophages are actively involved in recognizing, capturing, and destroying pathogens, as well as removing cellular debris. The most important role of macrophages is to initiate and regulate the inflammatory response: they synthesize and secrete a wide range of proinflammatory cytokines that activate other cells of the immune system and promote the development of inflammation. The functional state of macrophages directly depends on the work of mitochondria - not only as energy sources, but also as key participants in signaling pathways associated with the production of reactive oxygen species and regulation of the inflammasome. Their functional state depends on mitochondria, which are not only energy producers but also regulators of signaling pathways, including reactive oxygen species generation and inflammasome activation. Mitochondrial dysfunction can lead to excessive macrophage activation and chronic inflammation, typical of diseases like atherosclerosis and metabolic disorders. Damaged mitochondria release components such as mtDNA and cardiolipin, potentially triggering autoimmune responses. To prevent this, cells utilize mitophagy, a selective autophagy process that removes dysfunctional mitochondria via the lysosomal pathway. Polyunsaturated fatty acids are known to influence inflammation and mitochondrial function, including mitophagy. Arachidonic acid, a precursor of prostaglandins and leukotrienes, modulates immune responses, but its role in mitophagy remains unclear. The aim of this study was to investigate whether arachidonic acid affects mitophagy and the proinflammatory response of human macrophages. Primary monocytes were isolated from whole blood of healthy donors and differentiated into macrophages over 5 days. Cells were treated with 20 μM arachidonic acid for 24 hours, followed by 1 μg/ml LPS stimulation for another 24 hours. Cytokine secretion (TNF, IL6, IL8, CCL2) was measured by ELISA. Mitophagy was assessed using confocal microscopy by evaluating colocalization of mitochondrial and lysosomal dyes. The results showed that arachidonic acid enhanced mitophagy and reduced secretion of TNF, IL6, and CCL2 in response to LPS. These findings suggest that activation of mitophagy may contribute to the anti-inflammatory effects of arachidonic acid in macrophages.

About the authors

Alexander D Zhuravlev

Research Institute of General Pathology and Pathophysiology, Moscow, Russia

Email: Zhuravel17@yandex.ru
ORCID iD: 0000-0002-0451-2594
SPIN-code: 7309-2433
Scopus Author ID: 57391753500
ResearcherId: CAJ-4942-2022

Junior Researcher Fellow of Laboratory of Angiopathology

Russian Federation, 8, Baltiyskaya st., 125315, Moscow, Russia

Nikita G Nikiforov

Research Institute of General Pathology and Pathophysiology, Moscow, Russia;
Institute of Gene Biology, Russian Academy of Sciences, Moscow, Russia;
Russian Academy of Sciences, Moscow, Russia

Email: nikiforov.mipt@googlemail.com
ORCID iD: 0000-0002-2082-2429

PhD, Leading Researcher of Institute of General Pathology and Pathophysiology; Senior Researcher of Institute of Gene Biology of Russian Academy of Science; Senior Engineer of Engelhardt Institute of Molecular Biology

Russian Federation, 8, Baltiyskaya st., 125315, Moscow, Russia; 34/5 Vavilova Street, 119334, Moscow, Russia; 32, Vavilov street, 119991, Moscow, Russia

Svetlana S Verkhova

Research Institute of General Pathology and Pathophysiology, Moscow, Russia;
FSBSI "Petrovsky National Research Centre of Surgery", Moscow, Russian Federation

Email: verxova.svetlana@gmail.com
ORCID iD: 0000-0002-7953-0586

Senior Assistant of Laboratory of Angiopathology; PhD student of Laboratory of Cellular and Molecular Pathology of the Cardiovascular System

Russian Federation, 8, Baltiyskaya st., Moscow, Russia, 125315; 3 Tsyurupy st., Moscow, Russia, 117418

Yegor E Yegorov

Russian Academy of Sciences, Moscow, Russia

Email: yegorov58@gmail.com
ORCID iD: 0000-0002-5990-4077

PhD, Prof, Leading Researcher of Laboratory of Cancer Cell Biology

Russian Federation, 32, Vavilov street, 119991, Moscow, Russia

Mariam Ekta Bagheri

FSBSI "Petrovsky National Research Centre of Surgery", Moscow, Russian Federation

Email: ms.bvgheri@gmail.com
Scopus Author ID: 0000-0001-7952-1068

PhD student, Junior Researcher of Laboratory of Cellular and Molecular Pathology of the Cardiovascular System

Russian Federation, 3 Tsyurupy st., Moscow, Russia, 117418

Alexander N Orekhov

Research Institute of General Pathology and Pathophysiology, Moscow, Russia

Author for correspondence.
Email: alexandernikolaevichorekhov@gmail.com
ORCID iD: 0000-0002-3318-4681

PhD, Prof., The Head of Laboratory of Angiopathology

Russian Federation, 8, Baltiyskaya st., 125315, Moscow, Russia

References

  1. Dabravolski S.A., Nikiforov N.G., Zhuravlev A.D., Orekhov N.A., Grechko A.V., Orekhov A.N. Role of the mtDNA Mutations and Mitophagy in Inflammaging. Int. J. Mol. Sci. 2022. V. 23. P. 1323.
  2. Orekhov A.N., Nikiforov N.G., Omelchenko A.V., Sinyov V.V., Sobenin I.A., Vinokurov A.Y., Orekhova V.A. The Role of Mitochondrial Mutations in Chronification of Inflammation: Hypothesis and Overview of Own Data. Life (Basel). 2022. V. 12. P. 1153.
  3. Djuricic I., Calder P.C. Beneficial Outcomes of Omega-6 and Omega-3 Polyunsaturated Fatty Acids on Human Health: An Update for 2021. Nutrients. 2021. V. 13. P. 2421.
  4. Yang B., Zhou Y., Wu M., Li X., Mai K., Ai Q. ω-6 Polyunsaturated fatty acids (linoleic acid) activate both autophagy and antioxidation in a synergistic feedback loop via TOR-dependent and TOR-independent signaling pathways. Cell. Death. Dis. 2020. V. 11. P. 607.
  5. Zhang Y., Chen H., Zhang W., Cai Y., Shan P., Wu D., Zhang B., Liu H., Khan Z.A., Liang G. Arachidonic acid inhibits inflammatory responses by binding to myeloid differentiation factor-2 (MD2) and preventing MD2/toll-like receptor 4 signaling activation. Biochim. Biophys. Acta Mol. Basis. Dis. 2020. V. 1866. P. 165683.
  6. Hung H.C., Tsai S.F., Chou H.W., Tsai M.J., Hsu P.L., Kuo Y.M. Dietary fatty acids differentially affect secretion of pro-inflammatory cytokines in human THP-1 monocytes. Sci. Rep. 2023. V. 13. P. 5511.
  7. Jayatunga D.P.W., Hone E., Khaira H., Lunelli T., Singh H., Guillemin G.J., Fernando B., Garg M.L., Verdile G., Martins R.N. Therapeutic Potential of Mitophagy-Inducing Microflora Metabolite, Urolithin A for Alzheimer's Disease. Nutrients. 2021. V. 13. P. 3744.
  8. Liu M., Lu J., Yang S., Chen Y., Yu J., Guan S. Alliin alleviates LPS-induced pyroptosis via promoting mitophagy in THP-1 macrophages and mice. Food. Chem. Toxicol. 2022. V. 160. P. 112811.
  9. Luo T., Jia X., Feng W.D., Wang J.Y., Xie F., Kong L.D., Wang X.J., Lian R., Liu X., Chu Y.J., Wang Y., Xu A.L. Bergapten inhibits NLRP3 inflammasome activation and pyroptosis via promoting mitophagy. Acta. Pharmacol. Sin. 2023. V. 44. P. 1867-1878.
  10. Patoli D., Mignotte F., Deckert V., Dusuel A., Dumont A., Rieu A., Jalil A., Van Dongen K., Bourgeois T., Gautier T., et al. Inhibition of mitophagy drives macrophage activation and antibacterial defense during sepsis. J. Clin. Invest. 2020. V. 130. P. 5858-5874.
  11. Wasner K., Smajic S., Ghelfi J., Delcambre S., Prada-Medina C.A., Knappe E., Arena G., Mulica P., Agyeah G., et al. Parkin Deficiency Impairs Mitochondrial DNA Dynamics and Propagates Inflammation. Mov. Disord. 2022. V. 37. P. 1405-1415.
  12. Nikiforov N.G., Chegodaev Y.S., Zhuravlev A.D., Vysokikh M., Marey M., Grechko A.V., Popov M.A., Bagheri Ekta M., Orekhov A.N. Inflammatory stimulation of monocyte-macrophages inhibits mitophagy. Minerva Biotechnol. Biomol. Res. 2023. V. 35 № 3. P. 145-50.

Supplementary files

Supplementary Files
Action
1. JATS XML
Download

Copyright (c) Zhuravlev A.D., Nikiforov N.G., Verkhova S.S., Yegorov Y.E., Bagheri M.E., Orekhov A.N.

Creative Commons License
This work is licensed under a Creative Commons Attribution 4.0 International License.
СМИ зарегистрировано Федеральной службой по надзору в сфере связи, информационных технологий и массовых коммуникаций (Роскомнадзор).
Регистрационный номер и дата принятия решения о регистрации СМИ: серия ПИ № 77 - 11525 от 04.01.2002.


This website uses cookies

You consent to our cookies if you continue to use our website.

About Cookies