Cerebral venous disorders, including cerebral venous sinus stenosis (CVSS) and cerebral venous sinus thrombosis (CVST), can obstruct venous blood drainage, leading to intracranial hypertension. However, their effects on glymphatic function and white matter integrity in the brain remain poorly understood. Therefore, this study will enroll healthy controls, CVSS patients, and CVST patients to compare differences in glymphatic function and white matter microstructural integrity. Additionally, CVSS and CVST patients will undergo a 3-month follow-up to investigate the interrelationships and longitudinal changes among clinical parameters, glymphatic function, and white matter integrity.
Previously, researchers widely believed that the brain lacked a dedicated lymphatic system for clearing metabolic byproducts and wastes. However, recent studies have confirmed the existence of the glymphatic system along perivascular spaces (PVS), which plays a crucial role in metabolic waste clearance, nutrient and neuroactive substance exchange, regulation of central immune responses, and maintenance of cerebral fluid homeostasis. Emerging evidence suggests that dilated draining veins, elevated venous pressure, and increased intracranial pressure may impede glymphatic flow. Consequently, downstream venous pressure alterations-such as local stenosis or thrombosis in cerebral venous sinuses and/or internal jugular veins-could affect parenchymal venule pressure and volume, thereby influencing glymphatic system dynamics. Preserved myelin integrity is essential for maintaining synchronized and efficient interregional neural communication. Demyelination compromises brain network integration. Diffusion tensor imaging (DTI), an advanced magnetic resonance imaging (MRI) technique for assessing white matter microstructure, can sensitively detect integrity changes. Our preliminary studies identified characteristic bilateral symmetrical cloudy white matter alterations in patients with cerebral venous sinus stenosis, predominantly in periventricular and centrum semiovale regions. However, the precise pathological mechanism remains unclear, and direct evidence linking these changes to chronic venous outflow obstruction is lacking. Although similar imaging findings have not been reported in cerebral venous thrombosis patients, DTI may reveal early microstructural damage, suggesting potential pathological connections. White matter tracts serve not only as anatomical pathways for glymphatic flow but also depend on glymphatic clearance for metabolic homeostasis. This establishes a bidirectional regulatory relationship: glymphatic dysfunction may induce white matter injury, while white matter lesions could exacerbate glymphatic obstruction. Research indicates that glymphatic impairment may closely correlate with declining white matter integrity, with both potentially forming a mutually reinforcing feedback loop in disease progression across multiple pathologies. Therefore, this prospective cohort study aims to systematically evaluate glymphatic function and white matter integrity in cerebral venous diseases (including cerebral venous sinus stenosis and thrombosis), further exploring multidimensional correlations among clinical parameters, glymphatic activity, and white matter integrity. The findings may elucidate potential mechanisms of venous-related neural injury.
Study Type
OBSERVATIONAL
Enrollment
149
At baseline and day 90 (±14) post-enrollment: 1. Collect clinical data; 2. Administer multiple scales to assess clinical symptom severity and neuropsychological status; 3. Perform cranial diffusion tensor imaging (DTI) to evaluate glymphatic function and white matter integrity; 4. Collect peripheral blood and cerebrospinal fluid (CSF) samples for biomarker level analysis.
At baseline: 1. Collect clinical data; 2. Assess intracranial and extracranial arterial and venous systems; 3. Administer multiple scales to assess neuropsychological status; 4. Perform cranial diffusion tensor imaging (DTI) to evaluate glymphatic function and white matter integrity; 5. Collect peripheral blood samples for biomarker level analysis.
Xuanwu Hospital, Capital Medical University
Beijing, China
Change in DTI-ALPS index from baseline
The DTI-ALPS (Diffusion Tensor Imaging-Analysis along Perivascular Spaces) index is an imaging biomarker that quantitatively evaluates the function of the brain's glymphatic system using diffusion tensor imaging (DTI) technology, with lower values indicating impaired glymphatic clearance.
Time frame: day 90 (±14) post-enrollment
Change in PVS score from baseline
Perivascular spaces (PVS) in the basal ganglia (BG) and centrum semiovale (CSO) are visually scored as: 0 = none, 1 = 1-10, 2 = 11-20, 3 = 21-40, and 4 = \>40 on the axial slice with the highest burden and hemicerebrum with higher burden. An increase in PVS score implies a decrease in glymphatic function.
Time frame: day 90 (±14) post-enrollment
Change in PVS count from baseline
The number of PVS in the whole brain will be automatically calculated using deep learning algorithms. An increase in PVS count implies a decrease in glymphatic function.
Time frame: day 90 (±14) post-enrollment
Change in PVS volume from baseline
The volume of PVS in the whole brain will be automatically calculated using deep learning algorithms. An increase in PVS volume implies a decrease in glymphatic function.
Time frame: day 90 (±14) post-enrollment
Change in CPV from baseline
The choroid plexus volume (CPV) will be automatically segmented and calculated using Freesurfer software. An increase in CPV implies a decrease in glymphatic function.
Time frame: day 90 (±14) post-enrollment
Change in FA from baseline
Fractional anisotropy (FA) is obtained by Diffusion Tensor Imaging (DTI), and decreased FA values indicate white matter damage.
Time frame: day 90 (±14) post-enrollment
Change in MD from baseline
Mean diffusivity (MD) is obtained by Diffusion Tensor Imaging (DTI), and increased MD values indicate white matter damage.
Time frame: day 90 (±14) post-enrollment
Change in RD from baseline
Radial diffusivity (RD) is obtained by Diffusion Tensor Imaging (DTI), and increased RD values indicate white matter damage.
Time frame: day 90 (±14) post-enrollment
Change in AD from baseline
Axial diffusivity (AD) is obtained by Diffusion Tensor Imaging (DTI), and increased RD values indicate white matter damage.
Time frame: day 90 (±14) post-enrollment
Change in headache VAS score from baseline
The visual analogue scale (VAS) for headache assesses pain intensity on a 0-10 scale, where higher scores correlate with greater headache severity.
Time frame: day 90 (±14) post-enrollment
Change in HIT-6 score from baseline
Headache Impact Test-6 (HIT-6) is used to assess the comprehensive impact of headaches on quality of life, with total scores ranging from 36 to 78 points. Higher scores indicate greater disruption to daily functioning.
Time frame: day 90 (±14) post-enrollment
Change in tinnitus VAS score from baseline
The visual analogue scale (VAS) for tinnitus assesses symptom severity on a 0-10 scale, where higher scores indicate more severe tinnitus.
Time frame: day 90 (±14) post-enrollment
Change in THI score from baseline
The tinnitus handicap inventory (THI) is used to evaluate the impact of tinnitus on quality of life, with total scores ranging from 0 to 100. Higher scores reflect more severe disruption to daily functioning.
Time frame: day 90 (±14) post-enrollment
Change in head noise VAS score from baseline
The visual analogue scale (VAS) for head noise assesses symptom severity on a 0-10 scale, where higher scores indicate more severe head noise.
Time frame: day 90 (±14) post-enrollment
Change in HNHI score from baseline
Head noise handicap inventory (HNHI) is adapted from the tinnitus handicap inventory (THI) by systematically replacing "tinnitus" with "head noise" to evaluate the impact of head noise on quality of life. Total scores range from 0-100, with higher values reflecting more severe functional impairment.
Time frame: day 90 (±14) post-enrollment
Change in mRS score from baseline
Modified Rankin Scale (mRS) is used to assess neurological functional recovery status, with total scores ranging from 0 to 6. Higher scores indicate more severe neurological impairment and worse independent living capacity.
Time frame: day 90 (±14) post-enrollment
Change in HAMD-24 score from baseline
The 24-item Hamilton Depression Rating Scale (HAMD-24) is used to quantitatively assess the severity of depressive symptoms, with total scores ranging from 0 to 76. Higher scores indicate more severe depression.
Time frame: day 90 (±14) post-enrollment
Change in HAMA-14 score from baseline
The 14-item Hamilton Anxiety Rating Scale (HAMA-14) is used to quantitatively assess the severity of anxiety symptoms, with total scores ranging from 0 to 56. Higher scores indicate more severe anxiety.
Time frame: day 90 (±14) post-enrollment
Change in MMSE score from baseline
The Mini-Mental State Examination (MMSE) is used to assess cognitive function, with total scores ranging from 0 to 30. Lower scores indicate more severe cognitive impairment.
Time frame: day 90 (±14) post-enrollment
Change in MoCA score from baseline
The Montreal Cognitive Assessment (MoCA) is used to assess cognitive function, with total scores ranging from 0 to 30. Lower scores indicate more severe cognitive impairment.
Time frame: day 90 (±14) post-enrollment
Change in PSQI score from baseline
The Pittsburgh Sleep Quality Index (PSQI) is used to assess sleep quality, with total scores ranging from 0 to 21 points. A score \>5 points indicates sleep disturbance.
Time frame: day 90 (±14) post-enrollment
Change in fundus parameters from baseline
Fundus parameters include modified Frisen grading of the fundus, optic disc height, optic nerve sheath width, average retinal nerve fiber layer (RNFL) thickness, etc. These parameters to some extent reflect the degree of intracranial pressure.
Time frame: day 90 (±14) post-enrollment
Change in lumbar puncture opening pressure from baseline
The normal lumbar puncture opening pressure range for adults is 70-180 mmH₂O. A pressure \>200 mmH₂O typically indicates elevated intracranial pressure.
Time frame: day 90 (±14) post-enrollment
Change in Farb score from baseline
The Farb Score is used to evaluate the degree of venous sinus stenosis in subjects with cerebral venous sinus stenosis. The total score ranges from 0 to 8 points, with lower scores indicating higher degrees of stenosis.
Time frame: day 90 (±14) post-enrollment
Change in thrombus burden from baseline
The thrombus burden is measured semi-automatically using ITK-SNAP software on contrast-enhanced black-blood thrombus imaging of the head and neck veins.
Time frame: day 90 (±14) post-enrollment
Venous sinus recanalization rate
A three-tier classification based on contrast-enhanced MRV of the head and neck is used to evaluate venous sinus recanalization.
Time frame: day 90 (±14) post-enrollment
Change in biomarker levels in blood and cerebrospinal fluid from baseline
Blood and cerebrospinal fluid biomarkers include AQP4, Glial Fibrillary Acidic Protein (GFAP), Neurofilament Light Chain (NfL), Aβ40/42, total tau protein (Tau), phosphorylated tau181 (p-Tau181), interleukin (IL)-1β, IL-6, IL-8, IL-10, and tumor necrosis factor (TNF-α).
Time frame: day 90 (±14) post-enrollment
Incidence of adverse events
Adverse events included bleeding complications, major bleeding complications (hemoglobin drop ≥19 g/L), symptomatic intracranial hemorrhage, among others.
Time frame: day 90 (±14) post-enrollment
All-cause mortality
All-cause mortality refers to deaths from any cause within a studied population, regardless of the specific reason.
Time frame: day 90 (±14) post-enrollment
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