Per Wiik Johansen scite author profile

SummaryThe soluble branched yeast β β β β -1,3-D-glucan (SBG) belongs to a group of carbohydrate polymers known to exert potent immunomodulatory effects when administered to animals and humans. A new oral solution of SBG has been developed for local application to the oropharyngeal and oesophageal mucosa in order to strengthen the defence mechanisms against microbial and toxic influences. In the present study oral administration of SBG has been investigated primarily for assessment of safety and tolerability in an early phase human pharmacological study (phase I). Eighteen healthy volunteers were included among non-smoking individuals. The study was an open 1 : 1 : 1 dose-escalation safety study consisting of a screening visit, an administration period of 4 days and a follow-up period. Groups of six individuals received SBG 100 mg/day, 200 mg/day or 400 mg/day, respectively, for 4 consecutive days. The dose increase was allowed after a careful review of the safety data of the lower dose group. No drug-related adverse event, including abnormalities in vital signs, was observed. By inspection of the oral cavity only minor mucosal lesions not related to the study medication were seen in seven subjects. Repeated measurements of β β β β -glucan in serum revealed no systemic absorption of the agent following the oral doses of SBG. In saliva, the immunoglobulin A concentration increased significantly for the highest SBG dose employed. SBG was thus safe and well tolerated by healthy volunteers, when given orally once daily for 4 consecutive days at doses up to 400 mg.

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Pharmacokinetics of Perfluorobutane Following Intravenous Bolus Injection and Continuous Infusion of Sonazoid™ in Healthy Volunteers and in Patients with Reduced Pulmonary Diffusing Capacity

Landmark

Johansen

Johnson³

et al. 2008

Ultrasound in Medicine & Biology

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Pharmacokinetics of diltiazem and its metabolites in relation to CYP2D6 genotype

Molden

Johansen

Bøe

et al. 2002

Clin Pharma and Therapeutics

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CYP2D6 activity does not have a major impact on the disposition of diltiazem. In contrast, desacetyl diltiazem and N-demethyldesacetyl diltiazem are markedly accumulated in individuals expressing a deficient CYP2D6 phenotype. Because these metabolites exhibit pharmacologic properties of possible importance, individual CYP2D6 activity might be an aspect to consider in the clinical use of diltiazem.

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Reduced Platelet Function and Role of Drugs in Acute Gastrointestinal Bleeding

Kringen

Narum

Lygren

et al. 2010

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Gastrointestinal (GI) bleeding may be caused by a constitutive bleeding disposition or drug-induced inhibition of hemostasis. Platelet function in patients with ongoing GI bleeding is unknown. The aim of this study was to investigate platelet function in patients with acute GI bleeding. Patients (n = 35) presenting with acute GI bleeding (hematemesis or melena) were recruited. For comparison, 13 patients treated with aspirin and 11 patients treated with clopidogrel without GI bleeding and 27 healthy controls were studied. Platelet function was measured by whole-blood aggregation and flow cytometry. Coagulation function was measured with calibrated automated thrombography. Platelet aggregation and P-selectin expression were significantly lower after arachidonic acid stimulation in GI bleeding patients than in healthy subjects (p £ 0.05). Collageninduced P-selectin expression was significantly reduced in patients using anti-platelet drugs (p = 0.02) and in many patients not using anti-platelet drugs. Thrombin generation, measured by calibrated automated thrombography, was only reduced in patients on warfarin treatment. In conclusion, platelet function is reduced in acute GI bleeding patients and a considerable proportion appears to be related to drug use.Gastrointestinal (GI) bleeding has an incidence of 50 ⁄ 100,000 citizens per year [1], is often serious and even lethal. GI bleeding may be caused by inherited disposition, acquired bleeding diathesis, specific diseases such as Helicobacter pylori infection or oesophageal varices [2,3]. Acquired bleeding diathesis is often caused by adverse drug reaction of anti-thrombotic drugs. Both anti-coagulants and anti-platelet drugs are frequently used drugs in primary and secondary prevention of thromboembolism [4,5] and are associated with serious GI bleeding. Vitamin K antagonists, such as warfarin, interfere with the formation of functional gammacarboxylated vitamin K-dependent clotting factors (factors II, VII, IX and X) and anti-coagulants (protein C, -S and -Z) [6]. Aspirin and clopidogrel are the most commonly used anti-platelet drugs. Aspirin irreversibly acetylates cyclooxygenase (COX) -1 and inhibits thromboxane A2-mediated platelet aggregation as well as prostaglandin E 2 -mediated gastroprotection [7,8], whereas clopidogrel blocks the platelet adenosine diphosphate (ADP)-receptor P2Y 12 [9]. Non-steroidal anti-inflammatory drugs (NSAIDs) are frequently used non-selective and reversible inhibitors of both COX-1 and COX-2; however, the inhibition of COX-1 varies between the agents.Platelet count and platelet function are of vital importance for normal hemostasis. To our knowledge, no investigations have been published concerning platelet function in patients with acute GI bleeding. We hypothesized that in patients with acute GI bleeding, medications with known or possible influence on hemostasis cause a decrease in platelet and ⁄ or coagulation function. The aim of this study was therefore to investigate platelet function and the level of pro-coagulant...

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Regulation of Prolactin Secretion by Thyroliberin (TRH) in Cultured Rat Pituitary Tumor Cells

Gautvik¹,

Haug²,

Sand³

et al. 1984

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