Translocator protein (TSPO) genotype does not change cerebrospinal fluid levels of glial activation, axonal and synaptic damage markers in early Alzheimer's disease

被引:1
作者
Gouilly, Dominique [1 ]
Vrillon, Agathe [2 ,3 ]
Bertrand, Elsa [4 ]
Goubeaud, Marie [4 ]
Catala, Helene
Germain, Johanne [4 ]
Ainaoui, Nadera [4 ]
Rafiq, Marie [1 ,5 ]
Nogueira, Leonor [6 ]
Mouton-Liger, Francois
Planton, Melanie [1 ,5 ]
Salabert, Anne-Sophie [5 ,7 ]
Hitzel, Anne [7 ]
Meligne, Deborah [1 ,5 ]
Jasse, Laurence [1 ]
Sarton, Benjamine [5 ,8 ]
Silva, Stein [5 ,8 ]
Lemesle, Beatrice [1 ]
Peran, Patrice [5 ]
Payoux, Pierre [5 ]
Thalamas, Claire
Paquet, Claire
Pariente, Jeremie [1 ,4 ,5 ]
机构
[1] CHU Toulouse Purpan, Dept Cognit Neurol Epilepsy Sleep & Movement Diso, Toulouse, France
[2] Univ Paris, Hosp Lariboisiere Fernand Widal, AP HP, GHU Nord,Cognit Neurol Ctr, Paris, France
[3] Univ Paris, Therapeut Optimizat Neuropsychopharmacol, Inserm, UMRS11 44, Paris, France
[4] CHU Toulouse Purpan, Ctr Clin Invest, CIC 1436, Toulouse, France
[5] UPS, Toulouse Neuroimaging Ctr, Inserm, UMR 1214, Toulouse, France
[6] CHU Toulouse Purpan, Lab Cell Biol & Cytol, Toulouse, France
[7] CHU Toulouse Purpan, Dept Nucl Med, Toulouse, France
[8] CHU Toulouse Purpan, Crit Care Unit, Toulouse, France
关键词
TSPO; Neuro-inflammation; Rs6971; Cerebrospinal fluid; Alzheimer 's disease; VIVO RADIOLIGAND BINDING; NEUROINFLAMMATION; POLYMORPHISM; BRAIN; AD;
D O I
10.1016/j.nicl.2024.103626
中图分类号
R445 [影像诊断学];
学科分类号
100207 ;
摘要
Background: PET imaging of the translocator protein (TSPO) is used to assess in vivo brain inflammation. One of the main methodological issues with this method is the allelic dependence of the radiotracer affinity. In Alzheimer's disease (AD), previous studies have shown similar clinical and patho-biological profiles between TSPO genetic subgroups. However, there is no evidence regarding the effect of the TSPO genotype on cerebrospinalfluid biomarkers of glial activation, and synaptic and axonal damage. Method: We performed a trans-sectional study in early AD to compare cerebrospinal-fluid levels of GFAP, YKL-40, sTREM2, IL-6, IL-10, NfL and neurogranin between TSPO genetic subgroups. Results: We recruited 33 patients with early AD including 16 (48%) high affinity binders, 13 (39%) mixed affinity binders, and 4/33 (12%) low affinity binders. No difference was observed in terms of demographics, and cerebrospinal fluid levels of each biomarker for the different subgroups. Conclusion: TSPO genotype is not associated with a change in glial activation, synaptic and axonal damage in early AD. Further studies with larger numbers of participants will be needed to confirm that the inclusion of specific TSPO genetic subgroups does not introduce selection bias in studies and trials of AD that combine TSPO imaging with cerebrospinal fluid biomarkers.
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页数:6
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