Actively Recruiting

Age: 40Years - 85Years
All Genders
Healthy Volunteers
NCT05288842

Tanycytes in Alzheimer's Disease and Frontotemporal Dementia

Led by University Hospital, Lille · Updated on 2025-05-14

102

Participants Needed

1

Research Sites

212 weeks

Total Duration

On this page

Sponsors

U

University Hospital, Lille

Lead Sponsor

E

European Research Council

Collaborating Sponsor

AI-Summary

What this Trial Is About

Metabolic and hormonal deregulations are both a risk factor and a hallmark of Alzheimer's disease (AD) and frontotemporal dementia (FTD), occurring early in the course of the disease. In FTD in particular, hyperorality and dietary changes are associated with metabolic and hormonal changes such as altered levels of the anorexigenic hormone leptin. The hypothalamus is a brain region that controls metabolism and hormonal systems. Hypothalamic function depends on its ability to sense peripheral signals. The hypothalamus sits on a circumventricular organ called the median eminence (ME) that puts it in contact with systemic blood circulation. In the ME, fenestrated capillaries allow the diffusion of bloodborne factors. However, despite the lack of blood-brain barrier at brain microvessels, diffusion is controlled by specialized ependymoglial cells, the tanycytes, which exert a barrier function between the ME and the third ventricle and controls the access of blood-borne molecules into the hypothalamus. Previous work from our laboratory and the ERC consortium has highlighted the role of tanycytes not only in the regulation of the release of neurohormones from neuroendocrine nerve terminals into the pituitary portal blood circulation, but also in the transport of circulating leptin into the hypothalamus. Hence hypothalamic dysfunction in AD and FTD can result either from dysregulation of neuroendocrine secretions, direct neuronal loss or from defective transport (and hence resistance) to hormones like leptin. This study is to demonstrate that leptin transport though tanycytes is early altered in FTD and AD and correlates

CONDITIONS

Official Title

Tanycytes in Alzheimer's Disease and Frontotemporal Dementia

Who Can Participate

Age: 40Years - 85Years
All Genders
Healthy Volunteers

Eligibility Criteria

Eligible

You may qualify if you...

  • Subjects able to undergo a lumbar puncture
  • Subjects registered with the French Social Security as required by French biomedical law
  • For controls: no memory complaints and normal cognitive function based on standard tests
  • For Alzheimer's Disease group: diagnosis of probable Alzheimer's disease dementia per NIA 2011 criteria, MMSE score of 16 or above, have a study partner, and able to give informed consent
  • For Frontotemporal Dementia group: diagnosis of probable frontotemporal dementia per FTDC 2011 criteria, MMSE score of 16 or above, have a study partner, and able to give informed consent
Not Eligible

You will not qualify if you...

  • Dementia caused by non-neurodegenerative diseases, including severe cerebrovascular risk
  • Contraindications to lumbar puncture or MRI
  • Body weight under 45 kg
  • Other neurodegenerative diseases such as Lewy body dementia or Parkinson's disease
  • Serious neurological disorders like brain tumor, stroke, epilepsy, hydrocephalus
  • Severe metabolic or endocrine disorders except stable hypothyroidism, controlled type 2 diabetes, or common dyslipidemia
  • Treatment with metformin
  • Active infections with HCV, HBV, or HIV
  • Significant clinical or laboratory abnormalities
  • Pregnancy, breastfeeding, or women of childbearing age without effective contraception
  • Excessive alcohol intake or drug abuse
  • Risk of non-compliance or inability to be contacted in emergencies

AI-Screening

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Trial Site Locations

Total: 1 location

1

Memory Resources and Research Center Lille

Lille, France, 59037

Actively Recruiting

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Research Team

T

Thibaud LEBOUVIER, MD,PhD

CONTACT

How is the study designed?

Study Type

OBSERVATIONAL

Masking

N/A

Allocation

N/A

Model

N/A

Primary Purpose

N/A

Number of Arms

3

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