MedPath

Multiomics Targeting Microbiome Associated Changes in Stroke Patients (StrokeMicroBiomics)

Completed
Conditions
Transient Ischemic Attack
Ischemic Stroke
Interventions
Diagnostic Test: Microbiome and Plasma Characterisation
Registration Number
NCT04315922
Lead Sponsor
Ludwig-Maximilians - University of Munich
Brief Summary

Preclinical research has established a convincing connection between changes in the gut microbiota composition and stroke outcome. However clinical data on the gut-brain axis, and its chronic characteristics, is sparse. Additional investigations in the context of ischemic stroke regarding the relationship between dysbiosis and functional changes of the microbiome, as characterized by the metabolome, are still required. The StrokeMicroBiomics study will offer insight into these mechanisms and offer new potential targets for therapeutic interventions.

The primary objective is the characterisation of gut dysbiosis in ischemic stroke patients in the acute phase after stroke and during a 3 month follow-up period.

The secondary objectives include the identification of dysregulated gut microbiome metabolites and key immune cell populations in addition to the clinical progression of the study participants during the 3 month follow-up period after disease onset.

Detailed Description

Results of experimental, preclinical studies suggest that microbiome-targeted may improve stroke outcome as well as stroke-related comorbidities. Yet, clinical trials describing the extent and time course of microbiome changes after stroke are currently not available. Moreover, the impact of post-stroke dysbiosis on metabolic changes and the systemic immunity are unexplored.

Therefore, the primary objective of this trial is the characterization of gut dysbiosis progression in ischemic stroke patients during a 3 month follow-up period .

The secondary objectives include the identification of dysregulated gut microbiome metabolites and key immune cell populations in addition to the clinical progression of the study participants during the 3 month follow-up period after disease onset.

In order to elucidate the differential impact of lesion size on immune and microbiome homeostasis, separate patient cohorts with mild and severe stroke will be studied.

Furthermore, to control for the effects of temporary focal neurological deficits and stress induced microbiome and immune changes, patients with stroke mimics and transient ischemic attacks (TIA) are being recruited to the control group.

Recruitment & Eligibility

Status
COMPLETED
Sex
All
Target Recruitment
10
Inclusion Criteria
  • Written consent as submitted and approved to the human subjects review board must be gathered from the participants
  • Participants must be at least 50 years of age

For the severe stroke cohort, eligibility is defined by:

  • CT or MRI confirmed ischemic stroke affecting at least 1/3 of the anterior, medial or posterior cerebral arteries cortical coverage
  • NIHSS of at least 10 at time of induction into emergency room
  • Ischemic Stroke occured within the last 7 days

For the mild stroke cohort, eligibility is defined by:

  • CT or MRI confirmed ischemic stroke affecting no more than 1/3 of the anterior, medial or posterior cerebral arteries cortical coverage
  • NIHSS between 1 and 10 at time of induction into emergency room
  • Ischemic Stroke occured within the last 7 days

For the TIA cohort, eligibility is defined by:

  • CT or MRI confirmed absence of a lesion
  • NIHSS of 0 no more than 24 hours after induction into emergency room
  • TIA occured within the last 7 days
Exclusion Criteria
  • Pregnancy
  • Diagnosed and malignant Tumor ailment
  • Active, non-stroke related immunosuppression (i.e. HIV)
  • Infection, operative procedure or antibiotics treatment within 4 weeks prior to stroke/TIA
  • Relevant autoimmune disease (i.e Morbus Crohn)
  • Chronic infectious diseases (i.e Hepatitis C)
  • Hemorrhagic Stroke or intracranial bleeding
  • Cerebellar lesions
  • Other neurodegenerative diseases (i.e. Parkinson´s Disease or Alzheimers Dementia)

Study & Design

Study Type
OBSERVATIONAL
Study Design
Not specified
Arm && Interventions
GroupInterventionDescription
Mild Ischemic StrokeMicrobiome and Plasma CharacterisationMild Stroke as defined by inclusion criteria
Transient Ischemic AttackMicrobiome and Plasma CharacterisationTransient Ischemic Attack as defined by inclusion criteria
Severe Ischemic StrokeMicrobiome and Plasma CharacterisationSevere Stroke as defined by inclusion criteria
Primary Outcome Measures
NameTimeMethod
Changes from Baseline in the Gut Microbiome Composition at 3 Months post Stroke/TIA1-7 Days and 90 Days after Stroke

Gut Microbiome Composition is assessed using Shotgun Sequencing

Changes from Baseline of the Gut Metabolome as measured in Blood and Stool at 3 Months post Stroke/TIA1-7 Days and 90 Days after Stroke

The Metabolome is measured using Mass-Spectometry

Changes from Baseline in key Immune Populations at 3 Months post Stroke/TIA1-7 Days and 90 Days after Stroke

Immune Populations are measured using Flow Cytometry

Secondary Outcome Measures
NameTimeMethod
CT and (if available) MRI documentation1-7 days and 90 days after stroke
National Institute of Health Stroke Scale (NIHSS)1-7 days and 90 days after stroke
Modified Rankin Score (mRS)1-7 days and 90 days after stroke

Trial Locations

Locations (1)

LMU University hospital, Munich

🇩🇪

Munich, Bavaria, Germany

Related Trials

An Intervention Study Using HMOs to Improve IBS Symptoms

RecruitingNot Applicable
Glenn Gibson
Posted 2/28/2024
Updated 2/29/2024

Microbiome Benchmarking to Identify Perturbations in Multiple Sclerosis II

CompletedNot Applicable
National MS Center Melsbroek
Posted 1/9/2019
Updated 5/11/2022

Prebiotic and Probiotic Modulation of the Gut Microbiota-gut-brain Axis During Acute Stress

RecruitingNot Applicable
United States Army Research Institute of Environmental Medicine
Posted 5/26/2022
Updated 5/8/2024
© Copyright 2025. All Rights Reserved by MedPath
HomeTerms & ConditionsPrivacy Policy