| Literature DB >> 30054395 |
Zoltan Simandi1,2, Krisztian Pajer3, Katalin Karolyi1, Tatiana Sieler1, Lu-Lin Jiang4, Zsuzsanna Kolostyak2, Zsanett Sari2, Zoltan Fekecs3, Attila Pap2, Andreas Patsalos2, Gerardo Alvarado Contreras5, Balint Reho6, Zoltan Papp5, Xiufang Guo7, Attila Horvath2, Greta Kiss8, Zsolt Keresztessy2, György Vámosi6, James Hickman7, Huaxi Xu4, Dorothee Dormann9,10, Tibor Hortobagyi11, Miklos Antal8,12, Antal Nógrádi3, Laszlo Nagy13,2,14.
Abstract
Aging contributes to cellular stress and neurodegeneration. Our understanding is limited regarding the tissue-restricted mechanisms providing protection in postmitotic cells throughout life. Here, we show that spinal cord motoneurons exhibit a high abundance of asymmetric dimethyl arginines (ADMAs) and the presence of this posttranslational modification provides protection against environmental stress. We identify protein arginine methyltransferase 8 (PRMT8) as a tissue-restricted enzyme responsible for proper ADMA level in postmitotic neurons. Male PRMT8 knock-out mice display decreased muscle strength with aging due to premature destabilization of neuromuscular junctions. Mechanistically, inhibition of methyltransferase activity or loss of PRMT8 results in accumulation of unrepaired DNA double-stranded breaks and decrease in the cAMP response-element-binding protein 1 (CREB1) level. As a consequence, the expression of CREB1-mediated prosurvival and regeneration-associated immediate early genes is dysregulated in aging PRMT8 knock-out mice. The uncovered role of PRMT8 represents a novel mechanism of stress tolerance in long-lived postmitotic neurons and identifies PRMT8 as a tissue-specific therapeutic target in the prevention of motoneuron degeneration.SIGNIFICANCE STATEMENT Although most of the cells in our body have a very short lifespan, postmitotic neurons must survive for many decades. Longevity of a cell within the organism depends on its ability to properly regulate signaling pathways that counteract perturbations, such as DNA damage, oxidative stress, or protein misfolding. Here, we provide evidence that tissue-specific regulators of stress tolerance exist in postmitotic neurons. Specifically, we identify protein arginine methyltransferase 8 (PRMT8) as a cell-type-restricted arginine methyltransferase in spinal cord motoneurons (MNs). PRMT8-dependent arginine methylation is required for neuroprotection against age-related increased of cellular stress. Tissue-restricted expression and the enzymatic activity of PRMT8 make it an attractive target for drug development to delay the onset of neurodegenerative disorders.Entities:
Keywords: ADMA; CREB1; PRMT8; aging; motoneuron; neurodegeneration
Mesh:
Substances:
Year: 2018 PMID: 30054395 PMCID: PMC6113905 DOI: 10.1523/JNEUROSCI.3389-17.2018
Source DB: PubMed Journal: J Neurosci ISSN: 0270-6474 Impact factor: 6.167