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Downregulation of Scar Fibroblasts by Antineoplastic Drugs: A Potential Treatment for Fibroproliferative Disorders
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作者 m. georgina uberti Yvonne N. Pierpont +3 位作者 Rajat Bhalla Karan Desai martin C. Robson Wyatt G. Payne 《Surgical Science》 2016年第6期258-271,共14页
The various fibroproliferative disorders affecting humans have in common excess fibroblast activity and persistent overexpression or dysregulated activity of transforming growth factor beta (TGF-β). Cancer has many s... The various fibroproliferative disorders affecting humans have in common excess fibroblast activity and persistent overexpression or dysregulated activity of transforming growth factor beta (TGF-β). Cancer has many similar characteristics. Antineoplastic drugs can downregulate fibroblast activity and cytokine growth factors. This study evaluates the effect of six antineoplastic drugs on keloid and Dupuytren’s disease fibroblasts. Keloid, normal scar, Dupuytren’s affected palmar fascia, and normal palmar fascia fibroblasts were grown and seeded into Fibroblast Populated Collagen Lattices (FPCLs). The FPCLs were treated with one of six antineoplastic drugs or left untreated as controls. At 7 days, supernatants were extracted from all FPCLs and assayed for expression of Transforming Growth Factor beta (TGF)-β<sub>1</sub> and TGF-β<sub>2</sub>. All six antineoplastic drugs significantly inhibited FPCL contraction in both fibroproliferative conditions compared with the untreated controls (p β<sub>1</sub> and TGF-β<sub>2</sub> expression was downregulated in the supernatants of all FPCLs by the drug exposure. Cytotoxicity did not occur in these studies and was not the reason for the results. Although antineoplastic drugs can have significant side effects when given systemically, these results may be minimized when given to small areas involved in fibroproliferative scarring or when given topically or intralesionally. These in vitro results suggest that antineoplastic drugs may have a utility for treating various fibroproliferative disorders and warrant further investigation. 展开更多
关键词 Scar Fibroblasts Antineoplastic Drugs Fibroproliferative Disorders Dupuytren’s Disease KELOID
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背阔肌皮瓣乳房再造术设计算法(摘要)
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作者 Alan J. Durkin Yvonne N. Pierpont +8 位作者 Shitel Patel m. Lance Tavana m. georgina uberti Wyatt G. Payne David J. Smith Paul D. Smith 魏峰(译) 高景恒(译) 张晨(译) 《中国美容整形外科杂志》 CAS 2011年第3期I0020-I0020,共1页
目的肿瘤外科医师对手术技术的改进,使乳腺癌切除术后残留的乳房形态得到改善。以背阔肌皮瓣行乳房再造术效果肯定。本研究将评估不同类型的用于乳房再造术的背阔肌皮瓣的皮岛设计,寻找一种广泛用于修复各种乳腺癌切除术后缺损的背阔... 目的肿瘤外科医师对手术技术的改进,使乳腺癌切除术后残留的乳房形态得到改善。以背阔肌皮瓣行乳房再造术效果肯定。本研究将评估不同类型的用于乳房再造术的背阔肌皮瓣的皮岛设计,寻找一种广泛用于修复各种乳腺癌切除术后缺损的背阔肌皮瓣设计算法设计原则。方法本研究回顾性分析自2001年2月至2005年4月收治的单侧或双侧乳腺癌切除术后背阔肌皮瓣乳房再造患者的临床资料。在掌握如下情况的前提下进行再造手术:①术前组织是否经放疗处理;②体质量指数是否〉30;③当前有无吸烟习惯;④之前是否做过腹腔骨盆手术;⑤患者的要求。并对患者依据缺损形式进行分组:①乳房下皱襞完整但皮肤量不足;②乳房下皱襞完整且皮肤量足够;③乳房下皱襞缺损伴或不伴皮肤量不足。根据缺损的不同。设计不同的皮岛来优化手术效果,并减少供区瘢痕形成。结果本组患者54例,共应用64块背阔肌皮瓣行乳房再造术。各组间术后外观美学效果及供区瘢痕形成情况不同。结论本研究制定了一种背阔肌皮瓣乳房再造术的相关算法设计模式。通过对乳腺癌切除术后缺损的准确评价,在利用背阔肌皮瓣进行乳房再造术时,可定向切取皮岛,减少供区瘢痕形成,提高美学效果,获得疗效持久、外观自然、美观的乳房。 展开更多
关键词 乳房再造术 背阔肌皮瓣 皮岛设计 算法 双侧乳腺癌 乳房下皱襞 术后缺损 摘要
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