4.8 Article

Local IP3 receptor-mediated Ca2+ signals compound to direct blood flow in brain capillaries

SCIENCE ADVANCES (2021)

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Journal

SCIENCE ADVANCES
Volume 7, Issue 30, Pages -

Publisher

AMER ASSOC ADVANCEMENT SCIENCE
DOI: 10.1126/sciadv.abh0101

Keywords

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Categories

Multidisciplinary Sciences

Funding

  1. American Heart Association [14POST20480144, 17POST33650030, 20POST35210155, 17SDG33670237, 20CDA35310097, 19IPLOI34660108]
  2. Totman Medical Research Trust
  3. Fondation Leducq Transatlantic Network of Excellence on the Pathogenesis of Small Vessel Disease of the Brain
  4. European Union's Horizon 2020 Research and Innovation Programme [666881]
  5. Henry M. Jackson Foundation for the Advancement of Military Medicine [HU0001-18-2-0016]
  6. NIH [P01-HL-095488, R01-HL-121706, R37-DK-053832, 7UM-HL-1207704, R01-HL-131181, 4P20 GM103644/4-5, R24HL120847, R01HL120323]
  7. National Institute of Neurological Disorders and Stroke (NINDS)
  8. National Heart, Lung, and Blood Institute of the NIH [R35HL140027]
  9. Vermont Center for Cardiovascular and Brain Health [P20-GM-135007]
  10. University of California Irvine TMF Center [NCI-P30-CA062203]
  11. German Research Foundation (DFG) [FOR2372, KO 1582/10-1, KO 1582/10-2, KO 902/17-1, KO 902/17-2]
  12. National Institute on Aging (NIA) [R01NS110656, R01AG066645, DP2OD02944801]

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The study reveals that brain capillary endothelial cells control blood flow through a series of Ca2+ events, driven by neuronal activity and Ca2+ entry through TRPV4 channels. This provides a mechanism for high-resolution control of blood flow to small clusters of neurons.
Healthy brain function depends on the finely tuned spatial and temporal delivery of blood-borne nutrients to active neurons via the vast, dense capillary network. Here, using in vivo imaging in anesthetized mice, we reveal that brain capillary endothelial cells control blood flow through a hierarchy of IP3 receptor-mediated Ca2+ events, ranging from small, subsecond protoevents, reflecting Ca2+ release through a small number of channels, to high-amplitude, sustained (up to similar to 1 min) compound events mediated by large clusters of channels. These frequent (similar to 5000 events/s per microliter of cortex) Ca2+ signals are driven by neuronal activity, which engages G(q) protein-coupled receptor signaling, and are enhanced by Ca2+ entry through TRPV4 channels. The resulting Ca2+-dependent synthesis of nitric oxide increases local blood flow selectively through affected capillary branches, providing a mechanism for high-resolution control of blood flow to small clusters of neurons.

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