研究目的
To investigate the role of sphingosine 1-phosphate (S1P) in cerebral hemodynamics and oxygen metabolism and its neuroprotective effects against ischemic stroke.
研究成果
Elevated blood S1P improves cerebral blood oxygenation and reduces oxygen demand under hypoxia, providing neuroprotection against ischemic stroke when administered pre-treatment. Post-treatment is ineffective due to slow response times. This highlights the hemodynamic basis of S1P's neuroprotective effects and suggests potential for therapeutic development with improved pharmacokinetics.
研究不足
The study is limited to mouse models, which may not fully translate to humans. The SphK2 inhibitor has slow pharmacodynamics, limiting its effectiveness in post-treatment scenarios. Mechanisms of S1P clearance and specific roles in different blood components are not fully understood. General anesthesia was avoided, but skull thinning might cause minor inflammation.
1:Experimental Design and Method Selection:
The study used head-restrained multi-parametric photoacoustic microscopy (PAM) for high-resolution imaging of hemodynamics and oxygen metabolism in awake mice. A selective SphK2 inhibitor (SLM6031434) was used to increase blood S1P levels. Experiments included normoxia and hypoxia conditions, and transient middle cerebral artery occlusion (tMCAO) for stroke modeling.
2:Sample Selection and Data Sources:
CD-1 mice (male, 9–11 weeks old) from Charles River Laboratory were used. Blood samples were collected for S1P measurement via LC/MS.
3:List of Experimental Equipment and Materials:
Equipment includes PAM system with lasers (Edgewave BX40-2-G and BX40-2-GR), ultrasonic transducer, photodiode (Thorlabs SM1D12D), fiber (Thorlabs P1-460B-FC-2), lenses (Thorlabs AC127-025-A), head-restraint apparatus, rotarod for motor function test, laser Doppler flowmetry for occlusion confirmation, and LC/MS system (Shimadzu Prominence LC and AB Sciex 4000 QTRAP). Materials include SphK2 inhibitors (SLM6031434 and SLM6081442), isoflurane for anesthesia, dental cement (Parkell Inc. C&B Metabond), TTC for staining, and other chemicals.
4:Experimental Procedures and Operational Workflow:
Mice were prepared with skull thinning for PAM imaging. S1P levels were manipulated via intravenous injection of inhibitors. Hemodynamic parameters (CHb, sO2, CBF, CMRO2) were measured under normoxia and hypoxia. Stroke was induced by tMCAO, and outcomes (infarct volume, motor function, neurological deficit) were evaluated 24 hours post-stroke.
5:Data Analysis Methods:
Statistical analyses included two-way ANOVA, paired t-test, one-way ANOVA with Tukey's test, and unpaired t-test using software like ImageJ for infarct quantification.
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Laser
BX40-2-G
Edgewave
Optical excitation in the PAM system
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Laser
BX40-2-GR
Edgewave
Optical excitation in the PAM system
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Photodiode
SM1D12D
Thorlabs
Monitor laser energy to compensate for pulse-to-pulse fluctuation
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Fiber
P1-460B-FC-2
Thorlabs
Fiber coupling for laser beams
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Lens
AC127-025-A
Thorlabs
Achromatic doublet for optical alignment in PAM
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LC System
Prominence LC
Shimadzu
Liquid chromatography for S1P measurement
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Ultrasonic Transducer
Acoustic detection in PAM
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Mass Spectrometer
4000 QTRAP
AB Sciex
Triple quadrupole mass spectrometry for S1P quantification
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Dental Cement
C&B Metabond
Parkell Inc.
Adhere head plate to skull for restraint
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Nut
90730A005
McMaster-Carr
Part of head-restraint apparatus
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Filament
Beijing CiNongtech Co.
Occlude middle cerebral artery in tMCAO
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