Clinical Significance

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Abstract

Kitchener HC et al. Recurrent borderline tumors after conservative treatment management in women wishing to retain their fertility. Sukpan K et al. Mucinous tumor of low malignant potential ('borderline' or 'atypical proliferative' tumor) of the ovary: a study of 171 cases with the assessment of intraepithelial carcinoma and microinvasion. Ribassin-Majed L et al. Influence of histological subtypes on the risk of an invasive recurrence in a large series of stage I borderline ovarian tumor including 191 conservative treatments. Pathologic findings in eight cases of ovarian serous borderline tumors, three with foci of serous carcinoma, that preceded death or morbidity from invasive carcinoma. L et al. Age-dependent differences in borderline ovarian tumours (BOT) regarding clinical characteristics and outcome: results from a subanalysis of the Arbeitsgemeinschaft Gynaekologische Onkologie (AGO) ROBOT Study. Netupitant and palonosetron (NEPA): a winning team in the race for the optimal treatment of chemotherapy-induced nausea and vomiting? During the lifetime of many of healthcare professionals reading this article, the way in which chemotherapy induced nausea and vomiting (CINV) is approached and treated has transformed. The three papers reporting phase 2 and 3 dose-finding [1], efficacy and safety [1–3] studies of an oral fixed-dose combination (netupitant and palonosetron, NEPA) of a tachykinin NK 1 receptor [substance P (SP)] antagonist (NK 1 RA, netupitant, 300 mg) and a 5-hydroxytryptamine 3 receptor antagonist [5-HT 3 RA, palonosetron (PALO), 0.5 mg] are the latest clinical developments in the search for optimal anti-emetic therapy. This shift in approach to CINV is multifactorial: (i) a change in the attitude of healthcare professionals to nausea and vomiting, now viewed as something to be treated rather than tolerated by the patient; (ii) identification of risk factors initially: age, sex, alcohol consumption and emetic history, but screening for polymorphisms that may influence efficacy of 5-HT 3 RA (e.g. ABCB1, [4]) could be included; (iii) anti-emetic guidelines [5]; (iv) the introduction of the highly emetic cisplatin in the 1980s stimulated research into anti-emetics [6, 7]; (v) the recognition of anticipatory, acute and delayed phases of CINV [8] and insights into their differing mechanisms and pharmacology [9–11]; (vi) a shift in the way that identification of novel anti-emetics was approached by using models such as the ferret in which emesis was induced by cisplatin and which led to identification of the involvement of 5-The papers make three advances of note: (i) a single oral dose of NEPA on day 1 …
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临床意义
Kitchener等人。希望保留生育能力的妇女经保守治疗后复发的交界性肿瘤。Sukpan K等。卵巢低恶性潜能(“交界性”或“非典型增生性”肿瘤)粘液瘤:171例上皮内癌和微侵袭性评估的研究Ribassin-Majed L等人。组织学亚型对191例I期交界性卵巢肿瘤侵袭性复发风险的影响卵巢浆液性交界性肿瘤8例,其中3例伴浆液性癌灶,死亡或发病于浸润性癌。等等。交界性卵巢肿瘤(BOT)在临床特征和预后方面的年龄依赖性差异:来自Arbeitsgemeinschaft妇科肿瘤(AGO)机器人研究的亚分析结果。Netupitant和palonosetron (NEPA):在化疗引起的恶心和呕吐的最佳治疗竞赛中获胜的团队?在阅读本文的许多医疗保健专业人员的一生中,化疗引起的恶心和呕吐(CINV)的处理和治疗方式已经发生了变化。三篇关于速激肽NK 1受体[P物质(SP)]拮抗剂(NK 1 RA,奈妥吡坦,300 mg)和5-羟色胺3受体拮抗剂[5-HT 3 RA,帕洛诺司酮(PALO), 0.5 mg)口服固定剂量组合(奈妥吡坦和帕洛诺司酮,NEPA)的2期和3期剂量发现[1]、疗效和安全性[1 - 3]研究的论文是寻找最佳止吐疗法的最新临床进展。这种对CINV治疗方法的转变是多因素的:(i)医疗保健专业人员对恶心和呕吐的态度发生了变化,现在被视为需要治疗而不是患者容忍的事情;(ii)最初确定风险因素:年龄、性别、饮酒和呕吐史,但可能包括筛选可能影响5-HT - 3 RA疗效的多态性(例如ABCB1, [4]);(iii)止吐指南[5];(iv) 20世纪80年代引入的高催吐顺铂刺激了对止吐药的研究[6,7];(v)识别CINV的预期期、急性期和延迟期[8],并深入了解它们不同的机制和药理学[9-11];(vi)鉴定新型止吐剂的方法发生了转变,通过使用模型,如顺铂诱导呕吐的雪貂,从而确定了5的参与。论文提出了三个值得注意的进展:(i)第1天口服单剂量NEPA……
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