Ongoing studies Archive BIONIC, CAFE and SCALA

Please note: this study has been archived because participation is no longer possible or because it has been completed but is still temporarily available for viewing.


Goals

Diagnosis of cerebral amyloid angiopathy relies on criteria based on MRI markers. However, these are based on late and indirect markers and do not provide definitive proof of disease. This hampers early diagnosis. Thus, novel biomarkers are needed. Cerebrospinal fluid biomarkers are a proven option. read more

Goals

Diagnosis of  cerebral amyloid angiopathy relies on criteria based on MRI markers. However, these are based on late and indirect markers and do not provide definitive proof of the disease. This hampers early diagnosis. Thus, novel biomarkers are needed. Cerebrospinal  fluid biomarkers have proven to be a good option.

The need for new biomarkers of cerebral amyloid angiopathy

Several neuroimaging parameters have been proposed for diagnosing CAA in vivo. The most commonly used criteria are formulated in the 'Boston' criteria (see Table 1). The detection of large intraparenchymal hemorrhages on brain CT and MRI, in addition to small punctate hemorrhages (so called 'microbleeds', see Figure 1) or superficial collections of blood breakdown products within the brain grooves (so called 'superficial siderosis') detected on MRI, can be suggestive – but is not the final – proof for CAA . Besides, these abnormal findings on neuroimaging  represent only the very late stages of CAA. They should be regarded as the 'tip of the iceberg' of the true extent of CAA that is present in the brain.

Body fluid biomarkers

Thus, novel biomarkers are needed to accurately detect CAA. Cerebrospinal fluid (CSF) biomarkers may be an excellent candidate for the improved and early diagnosis of CAA, since CSF reflects the brain metabolic state and thus has the ability to reveal pathophysiological changes. For example, earlier work has demonstrated that the concentrations of two isoforms of amyloid β, i.e. amyloid β40 and amyloid β42, in CSF from CAA patients were decreased relative to controls and patients with Alzheimer’s disease.* In addition, we aim to find serum biomarkers.

Our research projects

In several research projects, we aim to develop and validate body fluid biomarkers  to provide diagnostic tools to clinicians that will allow them to detect CAA during life, to establish the contribution of CAA to cognitive decline and dementia, and to facilitate potential future personalized therapy. Currently active research project comprise:
  • BIONIC: BIOmarkers for cogNitive Impairment due to Cerebral amyloid angiopathy
  • SCALA: An Amyloid Beta Profile Specific for Cerebral Amyloid Angiopathy
  • CAFE: Cerebral amyloid angiopathy fluid biomarkers evaluation
* Verbeek MM, Kremer BP, Rikkert MO, Van Domburg PH, Skehan ME, Greenberg SM.Cerebrospinal fluid amyloid beta(40) is decreased in cerebral amyloid angiopathy.Ann Neurol. 2009 Aug;66(2):245-9. doi: 10.1002/ana.21694.

Figure 1: Example of typical MRI finding indicative of CAA: lobar microbleeds. The arrow indicates a lobar microbleed (SWI sequence).

Table 1: Modified Boston Criteria.

Background Cerebral Amyloid Angiopathy

What is CAA? How does it develop? And how can CAA be detected? read more

Background Cerebral Amyloid Angiopathy

What is CAA?

CAA is an important cause of cognitive decline or dementia and of cerebral hemorrhages in old age. It has a high prevalence (an estimated 10-50% of the general population), which increases with age. Also, approximately 80% of Alzheimer’s disease patients have CAA, the extent of which may vary considerably.

How does CAA develop?

The normal transport of amyloid β out of the brain parenchyma, across the so-called blood-brain barrier, towards the blood seems to be impaired. As a consequence, the amyloid β protein accumulates in the vessels of the brain. Once clinical symptoms become evident, CAA is already widespread in the brain, but at that time intervention is likely too late. Therefore, so-called biomarkers ('alarm signals') of early CAA development are clearly needed to improve early diagnosis and to stimulate the development of effective treatments.

How to detect CAA?

Currently, the definitive diagnosis of CAA can only be made by postmortem analysis of the brain tissue. Sensitive and specific diagnostic tests that allow detecting CAA during life are therefore dearly needed to allow for earlier detection and possible interventions.

Figure 1: Example of typical MRI finding indicative of CAA: lobar microbleeds. The arrow indicates a lobar microbleed (SWI sequence).
Figure 2: Immunohistochemical demonstration of amyloid β protein in CAA (anti-amyloid β staining).

Project leader

prof. dr. ir. Marcel Verbeek

+31 (0)24 361 45 67

Start and end date

  • Start date: 1 April 2018
  • End date: 1 April 2022

The projects


BIONIC project

Diagnosis of cerebral amyloid angiopathy (CAA) currently relies on the 'Boston criteria', which are based on MRI markers. However, these criteria are based on late and indirect hemorrhagic markers of CAA and do not provide definitive proof of the disease; this hampers early diagnosis. read more

CAFE project

Recently, a transgenic rat model of CAA was developed that closely resembles human CAA deposition in the microvasculature. This model allows for studying disease progression in relation to biomarker levels longitudinally, and gives the opportunity to investigate prodromal stages of disease. read more

SCALA project

This project aims to identify a profile of amyloid β-peptides in cerebrospinal fluid that is specific for CAA. If we manage to establish a CAA-specific profile of amyloid β peptide, this offers new possibilities for (early) diagnosis of CAA and monitoring the progression of the disease. read more

Grant providers

Team


External partner Leiden University Medical Center

Marieke Wermer PhD and Gisela Terwindt PhD.

External partner ADx Neurosciences

Hugo VanderStichele PhD.

External partner University of Gothenburg

Erik Portelius PhD.

External partner The University of Rhode Island

William E. Van Nostrand PhD.

Department Neurology

Our Neurological research focuses on neurodegenerative diseases like Parkinson's disease, Alzheimer's disease and child neurological diseases, and neuromuscular diseases like myopathies, channelopathies as well as cerebrovascular diseases like strokes and TIAs. read more