Your search keyword '"Damoiseaux, Jan G.M.C."' showing total 2 results

1. Plasma Dephosphorylated-Uncarboxylated Matrix Gla-Protein in Systemic Sclerosis Patients:Biomarker Potential for Vascular Calcification and Inflammation

Author

Potjewijd, Judith, Tobal, Rachid, Boomars, Karin A., van Empel, Vanessa V.P.M., de Vries, Femke, Damoiseaux, Jan G.M.C., Schurgers, Leon J., van Paassen, Pieter, Potjewijd, Judith, Tobal, Rachid, Boomars, Karin A., van Empel, Vanessa V.P.M., de Vries, Femke, Damoiseaux, Jan G.M.C., Schurgers, Leon J., and van Paassen, Pieter

Abstract

Background: Systemic sclerosis (SSc) patients face an elevated risk of cardiovascular disease (CVD), even when classic cardiovascular risk factors are considered. Plasma dephosphorylated-uncarboxylated Matrix Gla-protein (dp-ucMGP), an inactive form of MGP, is associated with increased CVD risk. Smooth muscle cells, implicated in SSc’s development, are the primary dp-ucMGP producers. This study assessed dp-ucMGP levels and initial CVD events in early-diagnosed SSc patients, investigating its potential as a CVD and all-cause mortality predictor over time. Methods:In a cohort of 87 SSc patients (excluding those with pre-existing CVD or on dialysis), baseline dp-ucMGP levels were measured, along with cardiovascular risk factors. Validation involved assessing dp-ucMGP in a subset of treatment-naive SSc patients. Results: A significantly elevated median dp-ucMGP level of 634 pmol/L (IQR 301) compared with healthy controls (dp-ucMGP < 393 pmol/L; p < 0.001) was observed. Validation in a treatment-naive SSc patient subset yielded similar results (median 589 pmol/L; IQR 370). During a median 10.5-year follow-up among 78 SSc patients, 33.3% experienced their first CVD event, independent of traditional risk factors. Elevated dp-ucMGP levels (>634 pmol/L) correlated with a higher risk of CVD and/or death (log-rank test: p < 0.01). Conclusions: In summary, dp-ucMGP emerges as a novel biomarker in SSc patients, with elevated levels indicating an increased risk of CVD and/or mortality in this population.

Published

2023

2. Autoimmune Encephalitis With mGluR1 Antibodies Presenting With Epilepsy, but Without Cerebellar Signs:A Case Report

Author

Vinke, Anita M., Zong, Shenghua, Janssen, Josien H., Correia-Hoffmann, Carolin, Mané-Damas, Marina, Damoiseaux, Jan G.M.C., de Vries, J. M., Pröpper, Dirk, Molenaar, Peter, Losen, Mario, Martinez Martinez, Pilar, Rouhl, Rob P.W., Vinke, Anita M., Zong, Shenghua, Janssen, Josien H., Correia-Hoffmann, Carolin, Mané-Damas, Marina, Damoiseaux, Jan G.M.C., de Vries, J. M., Pröpper, Dirk, Molenaar, Peter, Losen, Mario, Martinez Martinez, Pilar, and Rouhl, Rob P.W.

Abstract

OBJECTIVE: To describe the unique case history of a patient with mGluR1 antibodies, with mainly limbic and without cerebellar symptoms. METHODS: A 50-year-old woman initially presented with focal seizures with epigastric rising and déjà-vu sensations, next to cognitive complaints, and musical auditory hallucinations. MRI, EEG, and neuronal autoantibody tests were performed. RESULTS: EEG findings showed slow and sharp activity (sharp waves and sharp-wave-slow-wave complex) in the left temporal lobe. A test for autoantibodies was negative initially. Because of persistent symptoms, serum and CSF were tested 4 years later and found positive for mGluR1 antibodies. Treatment started with monthly IV immunoglobulins and azathioprine that was replaced by mycophenolate mofetil later. Especially cognitive symptoms and hallucinations did not respond well to the treatment. During treatment, mGluR1 antibodies remained present in CSF. DISCUSSION: Whereas cerebellar symptoms are present in 97% of mGluR1-positive cases, our patient presented without ataxia. Therefore, we suggest that the clinical presentation of patients with mGluR1 antibodies is probably more diverse than previously described. Testing for mGluR1 antibodies should be considered in patients with limbic encephalitis and epilepsy, especially when negative for more common antibodies.

Published

2022