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Mitochondria-Induced Immune Response as a Trigger for Neurodegeneration: A Pathogen from Within

INTERNATIONAL JOURNAL OF MOLECULAR SCIENCES (2021)

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Journal

INTERNATIONAL JOURNAL OF MOLECULAR SCIENCES
Volume 22, Issue 16, Pages -

Publisher

MDPI
DOI: 10.3390/ijms22168523

Keywords

mtDNA; mtRNA; mitochondrial dysfunction; mitochondrial disorders; neurodegeneration; antiviral response; inflammation; innate immunity; interferon

Categories

Biochemistry & Molecular Biology Chemistry, Multidisciplinary

Funding

  1. Juan de la Cierva grant [IJC2018-036938-I]
  2. European Research Council (Starting grant NEUROMITO) [ERC-2014-StG-638106]
  3. MINECO Proyectos I + D de Excelencia [SAF2014-57981P, SAF2017-88108-R]
  4. AGAUR [2017SGR-323]
  5. la Caixa Foundation [100010434, LCF/PR/HR20/52400018]

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The symbiosis between mitochondria and the ancestor of the eukaryotic cell is crucial for cellular complexity and survival, but compromised mitochondrial integrity can lead to unwanted cellular immune responses. Mitochondrial nucleic acids like mtDNA and mtRNA can interact with cytoplasmic sensors, triggering inflammation. Mitochondria-driven inflammation may serve as a potential therapeutic target for neurodegenerative and primary mitochondrial diseases.
Symbiosis between the mitochondrion and the ancestor of the eukaryotic cell allowed cellular complexity and supported life. Mitochondria have specialized in many key functions ensuring cell homeostasis and survival. Thus, proper communication between mitochondria and cell nucleus is paramount for cellular health. However, due to their archaebacterial origin, mitochondria possess a high immunogenic potential. Indeed, mitochondria have been identified as an intracellular source of molecules that can elicit cellular responses to pathogens. Compromised mitochondrial integrity leads to release of mitochondrial content into the cytosol, which triggers an unwanted cellular immune response. Mitochondrial nucleic acids (mtDNA and mtRNA) can interact with the same cytoplasmic sensors that are specialized in recognizing genetic material from pathogens. High-energy demanding cells, such as neurons, are highly affected by deficits in mitochondrial function. Notably, mitochondrial dysfunction, neurodegeneration, and chronic inflammation are concurrent events in many severe debilitating disorders. Interestingly in this context of pathology, increasing number of studies have detected immune-activating mtDNA and mtRNA that induce an aberrant production of pro-inflammatory cytokines and interferon effectors. Thus, this review provides new insights on mitochondria-driven inflammation as a potential therapeutic target for neurodegenerative and primary mitochondrial diseases.

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