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Introduction: Hip fracture surgery is associated with high in-hospital and 30-day mortality rates and serious adverse patient outcomes. Evidence from randomised controlled trials regarding effectiveness of spinal versus general anaesthesia on patient-centred outcomes after hip fracture surgery is sparse.
Methods and analysis: The iHOPE study is a pragmatic national, multicentre, randomised controlled, open-label clinical trial with a two-arm parallel group design. In total, 1032 patients with hip fracture (>65 years) will be randomised in an intended 1:1 allocation ratio to receive spinal anaesthesia (n=516) or general anaesthesia (n=516). Outcome assessment will occur in a blinded manner after hospital discharge and inhospital. The primary endpoint will be assessed by telephone interview and comprises the time to the first occurring event of the binary composite outcome of all-cause mortality or new-onset serious cardiac and pulmonary complications within 30 postoperative days. In-hospital secondary endpoints, assessed via in-person interviews and medical record review, include mortality, perioperative adverse events, delirium, satisfaction, walking independently, length of hospital stay and discharge destination. Telephone interviews will be performed for long-term endpoints (all-cause mortality, independence in walking, chronic pain, ability to return home cognitive function and overall health and disability) at postoperative day 30±3, 180±45 and 365±60.
Ethics and dissemination: iHOPE has been approved by the leading Ethics Committee of the Medical Faculty of the RWTH Aachen University on 14 March 2018 (EK 022/18). Approval from all other involved local Ethical Committees was subsequently requested and obtained. Study started in April 2018 with a total recruitment period of 24 months. iHOPE will be disseminated via presentations at national and international scientific meetings or conferences and publication in peer-reviewed international scientific journals.
Trial registration number: DRKS00013644; Pre-results
Das schmalblättrige Weideröschen, Epilobium angustifolium, zählt in Mitteleuropa zu den charakteristischen Pionierpflanzen auf Kahlschlagflächen und Waldrändern. Durch seine lange Blütezeit (Juni bis September) ist es für viele Blütenbesucher eine wichtige Pollen- und Nektarressource im ansonsten blütenarmen Spätsommer (MAURITZIO & SCHÄFER 1994). Zu seinen häufigsten Blütenbesuchern zählt die solitär lebende oligolektische Blattschneiderbiene Megachile lapponica. Sie sammelt Pollen nur an Pflanzen der Gattung Epilobium und bevorzugt dabei das schmalblättrige Weidenröschen (WESTRICH 1989). Aber auch Honigbienen, Apis mellifera, sind oft in großer Menge an diesen Blüten anzutreffen. Sie nutzen E. angustifolium vorwiegend als Nektarquelle (MAURITZIO & SCHÄFER 1994), sammeln aber auch Pollen auf den Blüten. Bei starkem Beflug durch die Honigbienen könnte es daher zu einer Verknappung der Ressource Pollen kommen. Dies könnte dazu führen, dass die Wildbienenweibchen für ihre Sammelflüge mehr Zeit und Energie aufwenden müssen. Im kritischen Fall einer Konkurrenz sollte auch die Aufzuchtrate und somit die Fitness von M. lapponica betroffen sein, deren Larven fast ausschließlich mit Epilobium-Pollen verpflegt werden. Auf einer Kahlschlagfläche im Kottenforst (Bonn) sollte untersucht werden, welche Insekten an den Blüten des schmalblättrigen Weidenröschens Pollen und/oder Nektar sammeln und welche Blütenbesucher gleichzeitig auch Blütenbestäuber sind. Vor allem aber sollte die Frage geklärt werden, ob es durch die Honigbiene zur Konkurrenz um den Pollen kommt.
Cysteinyl leukotriene receptor 1 antagonists (CysLT1RA) are frequently used as add-on medication for the treatment of asthma. Recently, these compounds have shown protective effects in cardiovascular diseases. This prompted us to investigate their influence on soluble epoxide hydrolase (sEH) and peroxisome proliferator activated receptor (PPAR) activities, two targets known to play an important role in CVD and the metabolic syndrome. Montelukast, pranlukast and zafirlukast inhibited human sEH with IC50 values of 1.9, 14.1, and 0.8 μM, respectively. In contrast, only montelukast and zafirlukast activated PPARγ in the reporter gene assay with EC50 values of 1.17 μM (21.9% max. activation) and 2.49 μM (148% max. activation), respectively. PPARα and δ were not affected by any of the compounds. The activation of PPARγ was further investigated in 3T3-L1 adipocytes. Analysis of lipid accumulation, mRNA and protein expression of target genes as well as PPARγ phosphorylation revealed that montelukast was not able to induce adipocyte differentiation. In contrast, zafirlukast triggered moderate lipid accumulation compared to rosiglitazone and upregulated PPARγ target genes. In addition, we found that montelukast and zafirlukast display antagonistic activities concerning recruitment of the PPARγ cofactor CBP upon ligand binding suggesting that both compounds act as PPARγ modulators. In addition, zafirlukast impaired the TNFα triggered phosphorylation of PPARγ2 on serine 273. Thus, zafirlukast is a novel dual sEH/PPARγ modulator representing an excellent starting point for the further development of this compound class.
The arachidonic acid cascade is a key player in inflammation, and numerous well-established drugs interfere with this pathway. Previous studies have suggested that simultaneous inhibition of 5-lipoxygenase (5-LO) and soluble epoxide hydrolase (sEH) results in synergistic anti-inflammatory effects. In this study, a novel prototype of a dual 5-LO/sEH inhibitor KM55 was rationally designed and synthesized. KM55 was evaluated in enzyme activity assays with recombinant enzymes. Furthermore, activity of KM55 in human whole blood and endothelial cells was investigated. KM55 potently inhibited both enzymes in vitro and attenuated the formation of leukotrienes in human whole blood. KM55 was also tested in a cell function-based assay. The compound significantly inhibited the LPS-induced adhesion of leukocytes to endothelial cells by blocking leukocyte activation.