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Clinical Trials/NCT05118217
NCT05118217
Unknown
Not Applicable

Retinal Microvascular Dysfunction in Non-Painful and Painful Diabetic Peripheral Neuropathy in Type 2 Diabetes Mellitus

University of Plymouth0 sites72 target enrollmentNovember 18, 2021
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ConditionsDiabetic Peripheral NeuropathyPainful Diabetic Neuropathy

Overview

Phase
Not Applicable
Intervention
Not specified
Conditions
Diabetic Peripheral Neuropathy
Sponsor
University of Plymouth
Enrollment
72
Primary Endpoint
Dynamic Vessel Analysis
Last Updated
4 years ago
OverviewInvestigatorsEligibility CriteriaOutcomesSimilar Trials

Overview

Brief Summary

This study primarily seeks to evaluate dysfunction of small blood vessels and their linkage to dysfunction of nerves in people with Type 2 Diabetes. The purpose of this research is to explore some of the underlying pathophysiology of diabetic peripheral neuropathy, particularly painful diabetic peripheral neuropathy. The pain experienced by individuals with painful diabetic peripheral neuropathy is severe and associated with low quality of life. The pain does not typically respond well to pharmacological management. The processes underpinning the sources of pain are poorly understood, consequently only around a third of patients benefit from existing treatments. Some historic research on the sources of pain suggest the retention of the ability to reduce blood flow in small vessels may underpin these pain pathways. This research aims to explore this possibility, looking at the nerve-linked response in small vessels with a flickering light within the eye.

Participants will complete three or four questionnaires: one demographic, two to aid with stratifying participants into groups concerning symptoms of neuropathy and an additional questionnaire if participants are stratified to the painful DPN group. A basic neurological examination of the feet will follow.

Basic measurements of height, weight and blood pressure will be recorded for each participant.

The primary sites of measurement of this small vessel dysfunction will be the eye and the foot investigated in a non-invasive manner. A bright flickering light will be shone into participants eyes, with the reaction of small vessels recorded. Sensors will also be placed on the feet and chest of participants and warmed to ~44C. An image will be taken of participants eyes to measure nerve layer thickness and an area of skin on the forearm will be illuminated to measure for levels of a metabolic marker. A picture of the eye will also be taken to determine nerve layer thickness.

Detailed Description

This cross-sectional observational study will take place between November 2021 and May 2022 and will recruit individuals with Type 2 Diabetes alongside painful or non-painful peripheral neuropathy. The study aims to determine the relationship between microvascular and metabolic markers and i) clinical neuropathy, ii) of painful neuropathy and iii) severity of neuropathic pain within a Type 2 Diabetic cohort. This will be done through achieving the following objectives: i) determination of whether retinal vasodilation in response to flicker-light stimulus is associated with i) the severity of neuropathy, ii) the presence of painful neuropathy and iii) severity of neuropathic pain within a T2DM cohort. ii) determination of whether levels of tissue-bound advanced glycation endproducts (AGEs) measured by skin autofluorescence are associated with i) the severity of neuropathy, ii) the presence of painful neuropathy and iii) severity of neuropathic pain within a T2DM cohort. iii) determination of whether pedal skin transcutaneous oxygen tension (TcPO2) measured by transcutaneous oximetry is associated with i) the severity of neuropathy, ii) the presence of painful neuropathy and iii) severity of neuropathic pain within a T2DM cohort. iv)determination of whether retinal nerve layer thickness is associated with the severity of neuropathy, the presence of painful neuropathy and severity of neuropathic pain within a T2DM cohort v)determination of whether the following factors are associated with the severity of neuropathy, the presence of painful neuropathy and severity of neuropathic pain within a T2DM cohort * HbA1c * Lipid profile * Body Mass Index * Blood Pressure

Registry
clinicaltrials.gov
Start Date
November 18, 2021
End Date
April 30, 2022
Last Updated
4 years ago
Study Type
Observational
Sex
All

Investigators

Responsible Party
Principal Investigator
Principal Investigator

Calvin Howorth

Principle Investigator/Lecturer of Podiatry

University of Plymouth

Eligibility Criteria

Inclusion Criteria

  • Participant is willing and able to give informed consent for participation in the study
  • Male or Female, aged 18 years or above.
  • Diagnosed with Type 2 Diabetes Mellitus (confirmed on clinical notes)
  • History of an abnormal neurovascular testing result (typically, 10g monofilament test)
  • Able (in the Investigators opinion) and willing to comply with all study requirements.
  • Willing to allow his or her General Practitioner and consultant, if appropriate, to be notified of participation in the study.
  • Must be willing to refrain from caffeine and tobacco consumption 24hrs before procedures are undertaken.
  • Participants must be willing and able (in the Investigator's opinion) to undertake DN4, Brief Pain Inventory-DPN and Michigan Neuropathy Screening Instrument questionnaires.
  • Able to lie flat

Exclusion Criteria

  • The participant may not enter the study if ANY of the following apply:
  • Patients with neuropathy due to other aetiological causes, such as hereditary, metabolic, inflammatory, cervical and lumbar spine diseases; cerebrovascular diseases; uremia; alcohol use; or toxic factors.
  • All patients with Type 1 diabetes.
  • A positive history of malignancy; connective tissue or infectious disease;
  • Deficiency of vitamin B12 or folate;
  • Chronic renal failure;
  • Liver failure;
  • Glaucoma;
  • Age-related macular degeneration
  • Epilepsy;

Outcomes

Primary Outcomes

Dynamic Vessel Analysis

Time Frame: during the procedure

Retinal vasodilation in response to flicker light stimulus - Response will be recorded as baseline corrected flicker response (bFR). Baseline will be recorded as the period from -30 to -5 seconds prior to flicker light stimulation. bFR will be calculated as the difference between peak dilation after provocation (dil%) and the minimum of the subsequent reactive constriction (constr%) and the width of the baseline amplitude (width BL%).

Secondary Outcomes

  • Transcutaneous Oximetry(during the procedure)
  • Lipid Profile(pre-procedure)
  • Retinal Nerve Layer Thickness(during the procedure)
  • Skin Autofluorescence(during the procedure)
  • Body Mass Index(during the procedure)
  • Static Vessel Analysis(during the procedure)
  • Blood pressure(during the procedure)
  • HbA1c(pre-procedure)

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