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Background: SPECT is one of the most employed techniques in the diagnostic workup of idiopathic Parkinson’s disease (IPD). Despite its widespread use, the exact diagnostic accuracy of this technique in parkinsonian syndromes remains controversial. Methods: In this study, we investigated the diagnostic accuracy of an initial ¹²³I-ioflupane (FP-CIT) and/or ¹²³I-iodobenzamide (IBZM) SPECT to differentiate between IPD and other parkinsonian disorders. 248 patients underwent a SPECT scan because of an as yet unclassified parkinsonian syndrome in our clinic between 2001 and 2006. Gold standard was the clinical diagnosis derived from the latest available clinical record, or, when this was not possible, a new complete physical and neurological examination by a blinded movement disorder specialist neurologist. Mean follow-up between SPECT and the latest clinical information was 18 months (range 3 months to 5 years). Results: 223 of the 248 patients were clinically definitely diagnosed after follow-up: IPD 127, atypical parkinsonian syndromes (APS) 27, essential tremor (ET) 22, vascular parkinsonism (VP) 16, drug-induced parkinsonism (DIP) 5, doubt between PD and APS 2, other diseases without dopaminergic involvement 24. The mean odds ratio (95% CI) for FP-CIT SPECT’s ability to distinguish between IPD and ET was 82 (11–674); between IPD and VP 61 (8–490); between IPD and DIP 36 (2–697) and between IPD and APS was 1 (0–4). The odds ratio for the IBZM SPECT tracer to differentiate between IPD and APS was 7 (2–17). Conclusions: FP-CIT SPECT is accurate to differentiate patients with IPD from those with ET, and IPD from VP and DIP. The accuracy of both FP-CIT and IBZM SPECT scans to differentiate between IPD and APS is low.

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The predictive value of transcranial duplex sonography for the clinical diagnosis in undiagnosed parkinsonian syndromes: comparison with SPECT scans

Vlaar

Nijs

Kroonenburgh

et al. 2008

BMC Neurol

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ApoB versus non-HDL-cholesterol: Diagnosis and cardiovascular risk management

Nijs

Sniderman

Graaf

2013

Critical Reviews in Clinical Laboratory Sciences

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The most recent guidelines released by the EAS/ESC and the Canadian Cardiovascular Society (CCS) retain low-density lipoprotein cholesterol (LDL-C) as the primary measure of the atherogenic risk of the apolipoprotein B (apoB) lipoproteins and the primary target of LDL-C lowering therapy. Both organizations endorse non-high-density lipoprotein cholesterol (non-HDL-C) and apoB as "alternate/secondary" targets, but neither group offers evidence supporting the continued preference of LDL-C as the primary target over non-HDL-C and apoB. Further, both suggest that non-HDL-C and apoB more or less measure the same thing and, therefore, are essentially interchangeable. But what is the evidence that LDL-C should remain the primary target, and are apoB and non-HDL-C mirror images of one another? Furthermore, are estimation of risk and establishment of treatment targets the only relevant issues, or is diagnosis also an essential objective? These are the questions this article will address. Our principal objectives are: (1) to clarify the differences between LDL-C, non-HDL-C, and apoB and to distinguish what they measure; (2) to summarize the evidence relating to LDL-C, non-HDL-C, and apoB as predictors of cardiovascular risk and as targets for treatment; and (3) to demonstrate that diagnosis of atherogenic dyslipoproteinemias should be a fundamental clinical priority.

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Isolated arterial calcifications of the lower extremities: A clue for NT5E mutation

Nijs

Albuisson

Ockeloen

et al. 2016

International Journal of Cardiology

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A forty-two year old man was referred to the Dept. of Vascular Medicine because of severe intermittent claudication of both legs, that started at the age of 27. He never smoked, used alcohol in moderation and didn't use illicit drugs. His medication included acetylsalicylic acid and rosuvastatin. His family history was unremarkable, notably with no atherosclerotic disease and no consanguinity. His medical history revealed pain in several small joints of the hands, knees, and ankles since 1994, without rheumatological diagnosis. Physical examination showed absent pulsations of the dorsal pedal arteries on both feet. Laboratory examination revealed normal serum concentration of total cholesterol (3.2 mmol/l), creatinine (71 μmol/l), glucose (5.3 mmol/l), calcium (2.41 mmol/l), inorganic phosphate (0.99 mmol/l), parathyroid hormone (4.3 pmol/l), and 25-OH-vitamin D (56 μmol/l). A CT angiography of the thorax and abdomen was performed in 2007 revealing extensive arterial lower limb calcifications starting from the femoral artery (Fig. 1). Remarkably, the aorta and coronary

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Digital Ischemia in a Young Woman after Minor Wrist Trauma—A Rare Diagnosis and an Innovative Multidisciplinary Treatment

Koeneman

Nijs

Rongen

et al. 2016

Journal of Vascular and Interventional Radiology

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Tjerk de Nijs

Diagnostic Value of <sup>123</sup>I-Ioflupane and <sup>123</sup>I-Iodobenzamide SPECT Scans in 248 Patients with Parkinsonian Syndromes

The predictive value of transcranial duplex sonography for the clinical diagnosis in undiagnosed parkinsonian syndromes: comparison with SPECT scans

ApoB versus non-HDL-cholesterol: Diagnosis and cardiovascular risk management

Isolated arterial calcifications of the lower extremities: A clue for NT5E mutation

Digital Ischemia in a Young Woman after Minor Wrist Trauma—A Rare Diagnosis and an Innovative Multidisciplinary Treatment

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