Coping mediates the influence of personality on life satisfaction in patients with rheumatic diseases

The accumulation of triglyceride-rich lipoproteins is an independent factor for an increased risk for premature arteriosclerosis. Common mutations in the lipoprotein lipase (LPL) gene are at least in part inherited susceptibility factors involved in the age- and sex-dependent phenotypic expression of hypertriglyceridemia. It can be estimated that about 20% of patients with hypertriglyceridemia are carriers of common LPL gene mutations (Asp9Asn, Asn291Ser, Trp86Arg, Gly188Glu, Pro207Leu, Asp250Asn) associated with the HLP. Genotyping of these LPL gene mutations is recommended especially in patients with high risk for premature arteriosclerosis. A comparably high number of individuals are carriers of common mutations (Ser447X) or silent mutations (Thr361) associated with low favorable lipids.

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Pharmacokinetics of rivaroxaban after bariatric surgery: a case report

Mahlmann

Gehrisch

Beyer‐Westendorf

2013

J Thromb Thrombolysis

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Rivaroxaban is a direct factor Xa inhibitor, which is rapidly absorbed in the upper gastrointestinal (GI) tract. In large trials, it has been shown to be effective and safe in VTE treatment. However, in these trials patients with morbid obesity were not reported and it is unknown if the standard dosage of 20 mg rivaroxaban is sufficient for bariatric patients, especially after bariatric surgery, which may impact the resorption of rivaroxaban. We report the case of a bariatric patient with high venous thromboembolism risk and instable INR after recent bariatric surgery, who was switched from Vitamin-K antagonists to rivaroxaban. After intake of 20 mg rivaroxaban, plasma concentration were repeatedly measured until 3 h after the second dose using a commercially available chromogenic aXa-assay. Furthermore, INR and aPTT were measured. Peak concentrations of 224.22 ng/ml were observed. After 6 h, plasma concentration decreased to 86.9 ng/ml and remained stable until 12 h (86.32 ng/ml). After 24 h, a trough level of 35.54 ng/ml was observed. The patients INR did immediately increase and remained significantly elevated throughout the day with a slow decrease. Since peak values of rivaroxaban plasma concentrations were in the expected range of published data, we conclude that resorption of rivaroxaban was immediate and not significantly impaired by bariatric surgery of the upper GI tract. Consequently, no dose adjustments seem to be necessary in this high-risk population.

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A 3-Day Delay in Synovial Fluid Crystal Identification Did Not Hinder the Reliable Detection of Monosodium Urate and Calcium Pyrophosphate Crystals

Tausche¹,

Gehrisch²,

Panzner³

et al. 2013

Journal of Clinical Rheumatology

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Frequency of Polymorphisms in the B-domain of Factor V Gene in APC-resistant Patients

Kostka¹,

Siegert²,

Schwarz³

et al. 2000

Thrombosis Research

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Successful eradication of acquired factor-VIII-inhibitor using single low-dose rituximab

Wermke¹,

Bonin²,

Gehrisch³

et al. 2009

Haematologica

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gastrointestinal symptoms to indicate progression of tissue damage. Serial evaluation of λ-FLC level showed an increase to 17.7 mg/dL by June 2008. She has thus relapsed with increased λ-FLC level and gastrointestinal amyloid deposits on a recent biopsy, but has refused a second ASCT. Serum FLC data indicate she remained in molecular remission for more than 18 months after her last bortezomib treatment.ASCT provides a substantial median survival in select AL patients, 8 but an over 25% mortality rate if even one organ has significant AL damage.8,9 Our data suggest treatments that improve end-organ damage should reduce transplant-related mortality, ultimately allowing a higher percentage of patients to undergo ASCT with improved outcomes.10 Bortezomib can reliably decrease serum FLC levels.11 In our 2 patients, we documented reversal of AL organ damage with what appears to be promising disease-free survival. Furthermore, Patient 1, who received a second transplant, has remained in remission for three years. This suggests that second transplants may result in improved outcomes by significantly decreasing the AL disease burden. Treatment with bortezomib-based therapy may result in hematologic and organ responses that would enable patients with endorgan damage who would have otherwise been precluded from transplantation to undergo ASCT.

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Standardized use of novel oral anticoagulants plasma level thresholds in a new thrombolysis decision making protocol

Kepplinger

Prakapenia

Barlinn

et al. 2015

J Thromb Thrombolysis

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Acute ischemic stroke (AIS) patients receiving non-vitamin-K antagonist oral anticoagulants (NOAC) are commonly excluded from thrombolytic therapy, as interpretation of coagulation tests remains unclear. We aimed to investigate the applicability of a novel institutional protocol for thrombolysis based on current expert recommendations and NOAC specific coagulation assessment. We included hospitalized AIS patients receiving NOAC for at least 24 h and consecutive AIS patients not receiving NOAC into a prospective study. We performed standard coagulation tests and specific tests for dabigatran, rivaroxaban and apixaban plasma levels. We studied 65 patients: mean age 72 ± 13 years, 30 (46 %) male, median NIHSS score 3 (IQR 6). Fifteen (23 %) were on NOAC treatment (5 dabigatran, 5 rivaroxaban, and 5 apixaban, respectively) and 50 (77 %) were not. In patients without NOAC, dabigatran was not detectable (0 ng/ml), and plasma levels of rivaroxaban (median: 10.0 ng/ml, IQR 7.0) and apixaban (7.2 ng/ml, IQR 6.7) were below our lower thresholds that allow thrombolysis. In patients with dabigatran pre-treatment, trough levels (58.0 ng/ml, IQR 143.0) were below our upper threshold that would allow thrombolysis in 3/5 patients. In patients receiving rivaroxaban, trough level (68.0 ng/ml, IQR 64.0) was below our predefined upper thresholds that would allow thrombolysis in 4/5 patients. In all patients on apixaban, trough level was above our predefined threshold of 40 ng/ml that precludes thrombolysis (98.2 ng/ml, IQR 84.3). Predefined thresholds of NOAC plasma levels in the decision of thrombolysis in NOAC treated AIS patients might supplement routine coagulation tests and should be validated in a larger study population.

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Venous Thrombosis After Long-haul Flights

Clinical importance of prothrombotic risk factors in pediatric patients with malignancy – impact of central venous lines

Common mutations of the lipoprotein lipase gene and their clinical significance

Pharmacokinetics of rivaroxaban after bariatric surgery: a case report

A 3-Day Delay in Synovial Fluid Crystal Identification Did Not Hinder the Reliable Detection of Monosodium Urate and Calcium Pyrophosphate Crystals

Frequency of Polymorphisms in the B-domain of Factor V Gene in APC-resistant Patients

Successful eradication of acquired factor-VIII-inhibitor using single low-dose rituximab

Standardized use of novel oral anticoagulants plasma level thresholds in a new thrombolysis decision making protocol

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