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1. Adverse events related to low dose corticosteroids in autoimmune hepatitis

Author

van den Brand, F.F., van der Veen, K.S., Lissenberg-Witte, B.I., Boer, Y.S. (Ynto) de, Hoek, B. (Bart) van, Drenth, J.P.H. (Joost), Verdonk, R.C. (Robert), Vrolijk, J.M. (Jan), Nieuwkerk, C.M.J. van, Bouma, G. (Gerben), van Gerven, N.M., Kuijvenhoven, J.P., Schreuder, T., Wouden, E.J. van der, van Meyel, J.J.M., Baak, L.C., Stadhouders, P., Klemt-Kropp, M., Verhagen, M., Bhalla, A., Ouden, J.W. (Jannie) den, Beuers, U. (Ulrich), van Erpecum, KJL, Buuren, H.R. (Henk) van, Brouwer, J.T. (johannes), van den Brand, F.F., van der Veen, K.S., Lissenberg-Witte, B.I., Boer, Y.S. (Ynto) de, Hoek, B. (Bart) van, Drenth, J.P.H. (Joost), Verdonk, R.C. (Robert), Vrolijk, J.M. (Jan), Nieuwkerk, C.M.J. van, Bouma, G. (Gerben), van Gerven, N.M., Kuijvenhoven, J.P., Schreuder, T., Wouden, E.J. van der, van Meyel, J.J.M., Baak, L.C., Stadhouders, P., Klemt-Kropp, M., Verhagen, M., Bhalla, A., Ouden, J.W. (Jannie) den, Beuers, U. (Ulrich), van Erpecum, KJL, Buuren, H.R. (Henk) van, and Brouwer, J.T. (johannes)

Abstract

Background: Autoimmune hepatitis requires long‐term therapy, and systemic cor‐ ticosteroids are the backbone of therapeutic management. Prolonged use of corti‐ costeroids may lead to adverse events but data from long‐term studies are mainly derived from studies in rheumatic diseases. Aim: To assess cataract, diabetes and fractures in relation to corticosteroid doses in the long‐term maintenance treatment of patients with autoimmune hepatitis. Methods: We retrospectively collected data on 476 patients (77% women) with an established diagnosis of autoimmune hepatitis. Binary logistic regression with a gen‐ eralised estimating equation was used to analyse the association between current corticosteroid use and the incidence of cataract, diabetes and fractures with onset after autoimmune hepatitis diagnosis. We corrected for sex, age, cirrhosis at diagno‐ sis and predniso(lo)ne use in the prior 3 years to account for possible ongoing effects. Results: A total of 6634 years, with a median of 13 (range 1‐40) per patient were recorded. The median age at diagnosis was 44 years (range 2‐88). Adverse events were documented in 120 (25%) patients. Low‐dose predniso(lo)ne (0.1‐5.0 mg/d) in‐ creased the odds of fractures whereas higher doses (>5.0 mg/d) increased the odds of cataracts and diabetes. Budesonide increased the odds of cataract and fractures; this effect was independent of predniso(lo)ne use in the prior 1, 2 or 3 years. Conclusions: Even low doses of corticosteroids frequently lead to substantial ad‐ verse events refuting the assumption that adverse events are prevented by adminis‐ tering low doses.

Published
2019
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2. Fluid hydration to prevent post-ERCP pancreatitis in average- to high-risk patients receiving prophylactic rectal NSAIDs (FLUYT trial): Study protocol for a randomized controlled trial

Author

Smeets, X.J.N.M. (Xavier J.N.M.), Da Costa, D.W. (David W.), Fockens, P. (Paul), Mulder, C.J.J. (Chris), Timmer, R. (Robin), Kievit, W. (Wietske), Zegers, M. (Marieke), Bruno, M.J. (Marco), Besselink, M.G. (Marc), Vleggaar, F.P. (Frank), Hulst, R.W.M. (René) van der, Poen, A.C. (Alexander), Heine, G.D.N. (Gerbrand D.N.), Venneman, N.G. (Niels), Kolkman, J.J. (Jeroen J.), Baak, L.C. (Lubbertus), Römkens, T.E.H., Dijk, S.M. (Sven) van, Hallensleben, N.D.L. (Nora D.L.), Vrie, W. (Wim) van de, Seerden, T.C.J. (Tom), Tan, A.C. (Adriaan), Voorburg, A.M.C.J. (Annet), Poley, J.-W. (Jan-Werner), Witteman, B.J.M. (Ben), Bhalla, A. (Abha), Hadithi, M. (Muhammed), Thijs, W.J., Schwartz, M.P. (Matthijs), Vrolijk, J.M. (Jan), Verdonk, R.C. (Robert), van Delft, F. (Foke), Keulemans, Y. (Yolande), Goor, H. (Harry) van, Drenth, J.P.H. (Joost), Geenen, E-J.M. (Erwin-Jan), Smeets, X.J.N.M. (Xavier J.N.M.), Da Costa, D.W. (David W.), Fockens, P. (Paul), Mulder, C.J.J. (Chris), Timmer, R. (Robin), Kievit, W. (Wietske), Zegers, M. (Marieke), Bruno, M.J. (Marco), Besselink, M.G. (Marc), Vleggaar, F.P. (Frank), Hulst, R.W.M. (René) van der, Poen, A.C. (Alexander), Heine, G.D.N. (Gerbrand D.N.), Venneman, N.G. (Niels), Kolkman, J.J. (Jeroen J.), Baak, L.C. (Lubbertus), Römkens, T.E.H., Dijk, S.M. (Sven) van, Hallensleben, N.D.L. (Nora D.L.), Vrie, W. (Wim) van de, Seerden, T.C.J. (Tom), Tan, A.C. (Adriaan), Voorburg, A.M.C.J. (Annet), Poley, J.-W. (Jan-Werner), Witteman, B.J.M. (Ben), Bhalla, A. (Abha), Hadithi, M. (Muhammed), Thijs, W.J., Schwartz, M.P. (Matthijs), Vrolijk, J.M. (Jan), Verdonk, R.C. (Robert), van Delft, F. (Foke), Keulemans, Y. (Yolande), Goor, H. (Harry) van, Drenth, J.P.H. (Joost), and Geenen, E-J.M. (Erwin-Jan)

Abstract

Background: Post-endoscopic retrograde cholangiopancreatography (ERCP) pancreatitis (PEP) is the most common complication of ERCP and may run a severe course. Evidence suggests that vigorous periprocedural hydration can prevent PEP, but studies to date have significant methodological drawbacks. Importantly, evidence for its added value in patients already receiving prophylactic rectal non-steroidal anti-inflammatory drugs (NSAIDs) is lacking and the cost-effectiveness of the approach has not been investigated. We hypothesize that combination therapy of rectal NSAIDs and periprocedural hydration would significantly lower the incidence of post-ERCP pancreatitis compared to rectal NSAIDs alone in moderate- to high-risk patients undergoing ERCP. Methods: The FLUYT trial is a multicenter, parallel group, open label, superiority randomized controlled trial. A total of 826 moderate- to high-risk patients undergoing ERCP that receive prophylactic rectal NSAIDs will be randomized to a control group (no fluids or normal saline with a maximum of 1.5 mL/kg/h and 3 L/24 h) or intervention group (lactated Ringer's solution with 20 mL/kg over 60 min at start of ERCP, followed by 3 mL/kg/h for 8 h thereafter). The primary endpoint is the incidence of post-ERCP pancreatitis. Secondary endpoints include PEP severity, hydration-related complications, and cost-effectiveness. Discussion: The FLUYT trial design, including hydration schedule, fluid type, and sample size, maximize its power of identifying a potential difference in post-ERCP pancreatitis incidence in patients receiving prophylactic rectal NSAIDs.

Published
2018
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5. The relation between plasma tyrosine concentration and fatigue in primary biliary cirrhosis and primary sclerosing cholangitis.

Author

Fekkes, D. (Durk), Vrolijk, J.M. (Jan), Buuren, H.R. (Henk) van, Borg, P.C.J. (Pieter) ter, Fekkes, D. (Durk), Vrolijk, J.M. (Jan), Buuren, H.R. (Henk) van, and Borg, P.C.J. (Pieter) ter

Abstract

BACKGROUND: In primary biliary cirrhosis (PBC) and primary sclerosing cholangitis (PSC) fatigue is a major clinical problem. Abnormal amino acid (AA) patterns have been implicated in the development of fatigue in several non-hepatological conditions but for PBC and PSC no data are available. This study aimed to identify abnormalities in AA patterns and to define their relation with fatigue. METHODS: Plasma concentrations of tyrosine, tryptophan, phenylalanine, valine, leucine and isoleucine were determined in plasma of patients with PBC (n = 45), PSC (n = 27), chronic hepatitis C (n = 22) and healthy controls (n = 73). Fatigue and quality of life were quantified using the Fisk fatigue severity scale, a visual analogue scale and the SF-36. RESULTS: Valine, isoleucine, leucine were significantly decreased in PBC and PSC. Tyrosine and phenylalanine were increased (p < 0.0002) and tryptophan decreased (p < 0.0001) in PBC. In PBC, but not in PSC, a significant inverse relation between tyrosine concentrations and fatigue and quality of life was found. Patients without fatigue and with good quality of life had increased tyrosine concentrations compared to fatigued patients. Multivariate analysis indicated that this relation was independent from disease activity or severity or presence of cirrhosis. CONCLUSION: In patients with PBC and PSC, marked abnormalities in plasma AA patterns occur. Normal tyrosine concentrations, compared to increased concentrations, may be associated with fatigue and diminished quality of life.

Published
2005
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6. The treatment of hepatitis C: history, presence and future

Author

Vrolijk, J.M. (Jan), Knegt, R.J. (Robert) de, Veldt, B.J. (Bart), Orlent, H. (Hans), Schalm, S.W. (Solko), Vrolijk, J.M. (Jan), Knegt, R.J. (Robert) de, Veldt, B.J. (Bart), Orlent, H. (Hans), and Schalm, S.W. (Solko)

Abstract

The treatment of chronic hepatitis C has made remarkable progress over the past two decades. For interferon-alpha monotherapy, sustained virological response rates were between 2 and 9% in genotype 1 and between 16 and 23% in genotypes 2 and 3. By adjusting treatment duration up to 48 weeks for genotype 1 and combining regular interferon-alpha with ribavirin, sustained response rates could be improved to 28 to 31% in genotype 1 and around 65% in genotypes 2 and 3. Attempts to further increase efficacy included the addition of amantadine without conclusive evidence up till now. With the recent introduction of long-acting pegylated interferon-alpha in combination with ribavirin, sustained virological response rates of 8o% can be obtained in genotypes 2 and 3. However, sustained virological response rates for patients with either genotype 1, nonresponse to prior treatment, cirrhosis or a combination of these characteristics are still less than 50%. In view of results with daily high-dose interferon-alpha induction in combination with prolongation of treatment duration up to 18 months, such patients might benefit from induction and prolonged PEG-IFN-alpha treatment and should be treated in an experimental setting.

Published
2004

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