Objectives: The diagnosis of glucose transporter-1 deficiency syndrome (GLUT-1 DS) can be challenging
due to the phenotypic heterogeneity among patients, coupled to confirmation that relies
on the one hand on a measure of cerebral spinal fluid (CSF) glucose concentration
typically reduced, but not always, and requires an invasive procedure. On the other
hand, genetic analysis of the SLC2A1 gene can lead to results which are difficult to interpret.
Background: The METAglut-1 blood test was able to detect a significantly lower expression of
GLUT-1 at the surface of red blood cells among 23 out of 30 patients tested who had
been diagnosed with the disease. The current study will allow a large-scale evaluation
of the test’s performance and has received a grant through the Forfait innovation
scheme from the French Ministry of Health and the High Authority for Health (Haute
Autorité de Santé, France).
Methods: When a patient presents clinical symptoms suggesting a GLUT-1 deficiency, a METAglut-1
test will be systematically performed blindly from the reference strategy consisting
in the measure of CSF glucose concentration complemented genetic analysis. The study
is multicentric and patients, children, and adults will be recruited in more than
40 centers all over France. The main goal will be to estimate the concordance between
the METAglut-1 test and CSF glucose concentration among all patients with a diagnostic
of certainty (either positive or negative) in the prospective cohort. Patients already
diagnosed can be included in a retrospective arm to strengthen exploratory the data.
A medical and economic analysis will be performed to evaluate the patients’ care pathway.
Conclusion: This study will allow to evaluate the diagnostic benefit of the METAglut-1 test and
its place in the diagnostic strategy of the GLUT-1 deficiency syndrome. The confirmation
of the high performance of the test will be very valuable as it only requires a simple
venous blood test, no need for fasting, and is characterized by a quick turnaround
time, to improve the early detection of patients which is of prime importance in this
neurological pathology for which efficient therapies are available.