TY - JOUR
T1 - Transfer RNA fragments replace microRNA regulators of the cholinergic poststroke immune blockade
AU - Winek, Katarzyna
AU - Lobentanzer, Sebastian
AU - Nadorp, Bettina
AU - Dubnov, Serafima
AU - Dames, Claudia
AU - Jagdmann, Sandra
AU - Moshitzky, Gilli
AU - Hotter, Benjamin
AU - Meisel, Christian
AU - Greenberg, David S.
AU - Shifman, Sagiv
AU - Klein, Jochen
AU - Shenhar-Tsarfaty, Shani
AU - Meisel, Andreas
AU - Soreq, Hermona
N1 - Publisher Copyright:
© 2020 National Academy of Sciences. All rights reserved.
PY - 2020/12/22
Y1 - 2020/12/22
N2 - Stroke is a leading cause of death and disability. Recovery depends on a delicate balance between inflammatory responses and immune suppression, tipping the scale between brain protection and susceptibility to infection. Peripheral cholinergic blockade of immune reactions fine-tunes this immune response, but its molecular regulators are unknown. Here, we report a regulatory shift in small RNA types in patient blood sequenced 2 d after ischemic stroke, comprising massive decreases of microRNA levels and concomitant increases of transfer RNA fragments (tRFs) targeting cholinergic transcripts. Electrophoresis-based size-selection followed by qRT-PCR validated the top six up-regulated tRFs in a separate cohort of stroke patients, and independent datasets of small and long RNA sequencing pinpointed immune cell subsets pivotal to these responses, implicating CD14+monocytes in the cholinergic inflammatory reflex. In-depth small RNA targeting analyses revealed the most-perturbed pathways following stroke and implied a structural dichotomy between microRNA and tRF target sets. Furthermore, lipopolysaccharide stimulation of murine RAW 264.7 cells and human CD14+monocytes up-regulated the top six stroke-perturbed tRFs, and overexpression of stroke-inducible tRF- 22-WE8SPOX52 using a single-stranded RNA mimic induced downregulation of immune regulator Z-DNA binding protein 1. In summary, we identified a "changing of the guards" between small RNA types that may systemically affect homeostasis in poststroke immune responses, and pinpointed multiple affected pathways, which opens new venues for establishing therapeutics and biomarkers at the protein and RNA level.
AB - Stroke is a leading cause of death and disability. Recovery depends on a delicate balance between inflammatory responses and immune suppression, tipping the scale between brain protection and susceptibility to infection. Peripheral cholinergic blockade of immune reactions fine-tunes this immune response, but its molecular regulators are unknown. Here, we report a regulatory shift in small RNA types in patient blood sequenced 2 d after ischemic stroke, comprising massive decreases of microRNA levels and concomitant increases of transfer RNA fragments (tRFs) targeting cholinergic transcripts. Electrophoresis-based size-selection followed by qRT-PCR validated the top six up-regulated tRFs in a separate cohort of stroke patients, and independent datasets of small and long RNA sequencing pinpointed immune cell subsets pivotal to these responses, implicating CD14+monocytes in the cholinergic inflammatory reflex. In-depth small RNA targeting analyses revealed the most-perturbed pathways following stroke and implied a structural dichotomy between microRNA and tRF target sets. Furthermore, lipopolysaccharide stimulation of murine RAW 264.7 cells and human CD14+monocytes up-regulated the top six stroke-perturbed tRFs, and overexpression of stroke-inducible tRF- 22-WE8SPOX52 using a single-stranded RNA mimic induced downregulation of immune regulator Z-DNA binding protein 1. In summary, we identified a "changing of the guards" between small RNA types that may systemically affect homeostasis in poststroke immune responses, and pinpointed multiple affected pathways, which opens new venues for establishing therapeutics and biomarkers at the protein and RNA level.
KW - Acetylcholine
KW - Immunology
KW - Ischemic stroke
KW - MicroRNA
KW - Transfer RNA fragment
UR - http://www.scopus.com/inward/record.url?scp=85098211863&partnerID=8YFLogxK
U2 - 10.1073/pnas.2013542117
DO - 10.1073/pnas.2013542117
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C2 - 33288717
AN - SCOPUS:85098211863
SN - 0027-8424
VL - 117
SP - 32606
EP - 32616
JO - Proceedings of the National Academy of Sciences of the United States of America
JF - Proceedings of the National Academy of Sciences of the United States of America
IS - 51
ER -