Birna ÁsbjörnsdóttirChristian Sandøe MusaeusMarie N. N. HellemTua Vinther-JensenPatrick EjlerskovEsben Budtz-JørgensenFilippa Liliendahl QvistAnja Hviid SimonsenLena E. HjermindNiels H. SkotteMarina Rode von EssenFinn SellebjergJørgen E. Nielsen
Background Blood-brain barrier (BBB) involvement in the pathogenesis of Huntington´s disease (HD) is not well understood. We previously demonstrated increased prevalence of T Helper 17.1 (Th17.1) cells in the cerebrospinal fluid (CSF) of HD gene-expansion carriers (HDGECs), which might indicate a dysfunction in the BBB or the blood-CSF barrier (BCB) in HD. Objective The aim of this exploratory study is to investigate whether the CSF/plasma albumin quotient (Q-Alb) and CSF platelet-derived growth factor-β (PDGFR-β) can be used as biomarkers for BBB/BCB integrity in HD and if there is an association between Q-Alb and the prevalence of intrathecal Th17.1 cells in HDGECs. Methods A total of 145 HDGECs and controls were included in the Q-Alb analysis. Forty-four of these individuals underwent a second lumbar puncture after five years and were included in the analysis of changes in Q-Alb over time. CSF from 33 HDGECs and controls was analysed for Th17.1 cells and CSF from 100 HDGECs and controls was analysed for PDGFR-β. Results No significant difference for Q-Alb was found between the pre-motor manifest HDGECs, motor manifest HDGECs, and controls (p = 0.49). We found a significant increase in Q-Alb in HDGECs over the 5-year period (p = 0.014), but when compared with controls, no significant difference was found (p = 0.32). No significant association was found between Q-Alb and the prevalence of Th17.1 cells (p = 0.97) nor Q-Alb and PDGFR-β (p = 0.89) in HDGECs. Conclusion We found no evidence of increased BBB/BCB leakage of albumin in HDGECs compared to controls. Neither did we find signs of pericyte involvement as measured by PDGFR-β in HDGECs. These results suggest that overt BBB/BCB disruption may be limited in HDGECs. Future longitudinal studies should employ more sensitive methods like dynamic contrast-enhanced magnetic resonance imaging to evaluate region specific microleaks.
Marina Rode von EssenMarie N.N. HellemTua Vinther‐JensenCecilie AmmitzbøllR. HansenLena E. HjermindTroels T. NielsenJørgen E. NielsenFinn Sellebjerg
Birna ÁsbjörnsdóttirChristian Sandøe MusaeusMarie NN HellemTua Vinther‐JensenLena E. HjermindAnja Hviid SimonsenMarina Rode von EssenFinn SellebjergJørgen E. Nielsen
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