Ear Cartilage

耳软骨
  • 文章类型: Journal Article
    目的:评估使用自体耳廓软骨(位于螺旋和反螺旋之间的前表面沟槽内)进行下睑牵开手术的疗效,并在患者队列中呈现手术结果。
    方法:回顾性分析了21例接受下睑后缩手术的患者的病历。回缩,存在时间延长(6个月至20年),表现为1毫米或更大的下巩膜显示,归因于之前的下眼睑眼睑成形术,面神经麻痹,或者作为正常的解剖变异。手术干预措施包括外侧than切开术,弯管溶解,睑下结膜-下眼睑牵开器的切口,下眼睑牵开器松解术,软骨移植物缝合到无结膜覆盖的缺损区域,并收紧所有患者的外侧角。
    结果:21例患者共29个眼睑行手术,术中无并发症。平均随访11个月(范围:6-30个月),96.5%的眼睑改善了下眼睑回缩。与术前相比,术后边缘到反射距离测量值(MRD2)显着降低(p=0.001;p<0.01)。MRD2-a(中瞳孔到下眼睑)和MRD2-b(外侧角膜缘到下眼睑)的平均改善分别为1.77±0.80和2.04±0.81(p=0.001;p<0.01)。四个眼皮(4/29)因眼角松动而需要翻修,矫正需要骨膜瓣。所有四名患者先前都曾在其他地方接受过两次或更多次修复。移植物在两个盖子上可见,但不需要进一步修改。一名患者在供体部位出现轻度螺旋畸形,这不需要额外的干预。
    结论:在下眼睑回缩与中/后板层缩短相关的情况下,利用自体耳骨软骨垫片移植提供了显着的好处。这些优点包括直接收获与最小的供体部位并发症,稳定而不经历收缩,与后软骨相比,质地更柔软,便于正确安装在地球仪上的凹形形状,和它的自体性质。
    OBJECTIVE: To assess the efficacy of lower eyelid retraction surgery utilizing autologous auricular scapha cartilage (located within the anterior surface groove between the helix and anti-helix) and to present the surgical outcomes in a patient cohort.
    METHODS: Medical records of 21 patients who underwent lower eyelid retraction surgery with scapha cartilage were retrospectively reviewed. Retractions, present for an extended duration (6 months to 20 years), exhibited 1 mm or more inferior scleral show, attributed to prior lower eyelid blepharoplasty, facial palsy, or as a normal anatomical variation. Surgical interventions included lateral canthotomy, cantholysis, incision of the subtarsal conjunctiva-lower eyelid retractors, lower eyelid retractor lysis, cartilage graft suturing to the defect area without conjunctival cover, and tightening of the lateral canthal corner in all patients.
    RESULTS: A total of 29 eyelids in 21 patients underwent surgery without intraoperative complications. Over a mean follow-up period of 11 months (range: 6-30 months), lower lid retraction improved in 96.5% of eyelids. Postoperative margin-to-reflex distance measurements (MRD2) significantly decreased compared to preoperative values (p = 0.001; p < 0.01). Average improvements in MRD2-a (midpupil to lower lid) and MRD2-b (lateral limbus to lower lid) were 1.77 ± 0.80 and 2.04 ± 0.81, respectively (p = 0.001; p < 0.01). Four eyelids (4/29) required revision due to canthal corner loosening, with correction necessitating periosteal flaps. All four patients had previously undergone two or more repairs elsewhere. The graft was visible in two lids but did not require further revision. One patient experienced mild helix deformity at the donor site, which did not warrant additional intervention.
    CONCLUSIONS: In cases of lower lid retraction associated with middle/posterior lamellar shortening, utilizing an autologous auricular scapha cartilage spacer graft offers notable benefits. These advantages comprise straightforward harvesting with minimal donor site complications, stability without experiencing shrinkage, a softer texture in comparison to posterior cartilage, a concave shape that facilitates proper fitting on the globe, and its autologous nature.
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  • 文章类型: Journal Article
    当前的组织工程方法利用主要来自肋部或关节来源的软骨细胞。尽管来自这些细胞的新软骨具有强大的机械性能,从这些来源收集的细胞缺乏弹性和侵入性对临床翻译产生负面影响。这些限制要求探索自然弹性耳廓软骨作为替代细胞来源。本研究旨在确定耳廓软骨细胞是否可用于无组织工程支架的新软骨构建体,并评估其生物力学特性。新软骨是从三个小型猪供体(N=3)的少量原代新生儿耳廓软骨细胞中成功产生的。新软骨构建体在10%和20%应变下的瞬时模量(Ei)为200.5kPa±43.34和471.9kPa±92.8,分别。TE构建体的弛豫模量(Er)在10%和20%应变下分别为36.99kPa±6.47Er和110.3kPa±16.99,分别。杨氏模量为2.0MPa±0.63,极限拉伸强度(UTS)为0.619MPa±0.177。耳廓软骨细胞来源的新软骨含有0.144ug±0.011胶原蛋白,0.185ug±0.002糖胺聚糖/ug干重,和每ug干重1.7e-3ug弹性蛋白。总之,这项研究表明,耳廓软骨细胞可以作为一种可靠且易于获得的细胞来源,用于仿生和机械坚固的弹性新软骨植入物的组织工程。
    Current tissue engineering (TE) methods utilize chondrocytes primarily from costal or articular sources. Despite the robust mechanical properties of neocartilages sourced from these cells, the lack of elasticity and invasiveness of cell collection from these sources negatively impact clinical translation. These limitations invited the exploration of naturally elastic auricular cartilage as an alternative cell source. This study aimed to determine if auricular chondrocytes (AuCs) can be used for TE scaffold-free neocartilage constructs and assess their biomechanical properties. Neocartilages were successfully generated from a small quantity of primary neonatal AuCs of three minipig donors (n = 3). Neocartilage constructs had instantaneous moduli of 200.5 kPa ± 43.34 and 471.9 ± 92.8 kPa at 10% and 20% strain, respectively. TE constructs\' relaxation moduli (Er) were 36.99 ± 6.47 kPa Er and 110.3 ± 16.99 kPa at 10% and 20% strain, respectively. The Young\'s modulus was 2.0 MPa ± 0.63, and the ultimate tensile strength was 0.619 ± 0.177 MPa. AuC-derived neocartilages contained 0.144 ± 0.011 µg collagen, 0.185 µg ± 0.002 glycosaminoglycans per µg dry weight, and 1.7e-3 µg elastin per µg dry weight. In conclusion, this study shows that AuCs can be used as a reliable and easily accessible cell source for TE of biomimetic and mechanically robust elastic neocartilage implants.
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  • 文章类型: Case Reports
    背景技术一名52岁男性患者在气管造口手术闭合26年后出现慢性咳嗽和持续气管刺激的症状,由自体耳廓软骨移植和皮肤移植支持。在最初的临床表现中,病人是个活跃的吸烟者,累积剂量为31包。病例报告支气管镜检查显示气管内毛发生长和移植部位局部炎症。初始抗炎,抗真菌药,进行了抗菌治疗,其次是内窥镜结构重塑。多次复发,症状相似,显示孤立的头发生长,没有炎症。指出了年度内窥镜重组会议,病人经历了他们的高度缓解。通过氩等离子体激光凝固和戒烟后,最终终止了头发的反复生长。我们假设头发生长的开始是由患者吸烟引发的。结论气管内毛发生长是自体移植支持的气管重建的潜在并发症。抗菌和抗炎药的初始给药,结合内镜重组,可能包含活动性炎症;氩等离子体激光凝固的应用最终阻止了头发的生长。吸烟与呼吸道上皮中分子信号通路的上调有关,可以刺激毛囊,比如刺猬蛋白,WNT-1/β-catenin,和表皮生长因子受体.
    BACKGROUND A 52-year-old male patient presented with symptoms of chronic cough and persistent tracheal irritation 26 years after surgical closure of a tracheostoma, supported by an autologous auricular cartilage graft and cutaneous transplant. At the initial clinical presentation, the patient was an active smoker, with a cumulative dose of 31 pack years. CASE REPORT Bronchoscopy revealed endotracheal hair growth and local inflammation at the graft site. Initial anti-inflammatory, antimycotic, and antibacterial therapy was administered, followed by endoscopic structure remodeling. There were multiple recurrences with similar symptoms, showing isolated hair growth, without inflammation. Annual endoscopic restructuring sessions were indicated, and the patient experienced them as highly relieving. Recurrent hair growth was finally terminated by argon plasma laser-coagulation and after smoking cessation. We hypothesize that the onset of hair growth was triggered by the patient\'s cigarette smoking. CONCLUSIONS Endotracheal hair growth is a potential complication of autograft-supported tracheal restructuring. The initial administration of antimicrobial and anti-inflammatory medication, combined with endoscopic restructuring, could have contained the active inflammation; the application of argon plasma laser-coagulation finally stopped the hair growth. Smoking is associated with the upregulation of molecular signaling pathways in the respiratory epithelium, which can stimulate hair follicles, such as sonic hedgehog protein, WNT-1/ß-catenin, and epidermal growth factor receptor.
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  • 文章类型: Journal Article
    背景:源自人脂肪间充质干细胞(hADSC)的细胞外囊泡(EV)在整形和重建手术中显示出巨大的治疗潜力。然而,电动汽车有限的生产和功能分子负载阻碍了其临床转化。hADSC的传统二维培养导致干细胞丧失和细胞衰老,这不利于电动汽车的生产和功能分子负载。再生医学的最新进展主张使用hADSCs的三维培养来生产电动汽车,因为它更准确地模拟他们的生理状态。此外,EV在组织工程中的成功应用依赖于将EV靶向递送到生物材料支架内的细胞.
    结果:利用hADSCs球体和hADSCs明胶甲基丙烯酸酯(GelMA)微球生产三维培养的电动汽车,分别对应于hADSCs球体-EV和hADSCs微球-EV。与hADSC微球-EV相比,hADSC球体-EV表现出优异的生产和功能分子负载。8种miRNA(即hsa-miR-486-5p,hsa-miR-423-5p,hsa-miR-92a-3p,hsa-miR-122-5p,hsa-miR-223-3p,hsa-miR-320a,hsa-miR-126-3p,和hsa-miR-25-3p)以及hADSC球体-EV中hsa-miR-146b-5p的下调显示出可能通过整合的调节机制改善剩余耳软骨细胞的命运并促进软骨形成的潜力。此外,开发了一种快速和创新的管道,用于从hADSC球体的三维动态培养物中分离软骨细胞归巢肽修饰的EV(CHP-EV)。CHP-EV是通过在外泌体表面蛋白LAMP2B的N末端遗传融合CHP而产生的。用波浪运动培养CHP+LAMP2B转染的hADSCs球体,以促进CHP-EV的分泌。使用收获方法来实现CHP-EV的时间依赖性收集。该管道易于设置,可快速用于CHP-EV的隔离。与未标记的电动汽车相比,CHP-EV穿透生物材料支架并特异性地将治疗性miRNA递送至剩余的耳软骨细胞。功能上,CHP-EV对促进细胞增殖具有重要作用,减少M1巨噬细胞浸润的微环境中剩余的耳软骨细胞的细胞凋亡并增强软骨形成。
    结论:总之,开发了一种创新的管道,从hADSC球体的三维动态培养中获得CHP-EV。该管道可以定制以增加电动汽车产量和功能分子负载,满足调节M1巨噬细胞浸润微环境中剩余的耳软骨细胞命运的要求。
    BACKGROUND: Extracellular vesicles (EVs) derived from human adipose-derived mesenchymal stem cells (hADSCs) have shown great therapeutic potential in plastic and reconstructive surgery. However, the limited production and functional molecule loading of EVs hinder their clinical translation. Traditional two-dimensional culture of hADSCs results in stemness loss and cellular senescence, which is unfavorable for the production and functional molecule loading of EVs. Recent advances in regenerative medicine advocate for the use of three-dimensional culture of hADSCs to produce EVs, as it more accurately simulates their physiological state. Moreover, the successful application of EVs in tissue engineering relies on the targeted delivery of EVs to cells within biomaterial scaffolds.
    RESULTS: The hADSCs spheroids and hADSCs gelatin methacrylate (GelMA) microspheres are utilized to produce three-dimensional cultured EVs, corresponding to hADSCs spheroids-EVs and hADSCs microspheres-EVs respectively. hADSCs spheroids-EVs demonstrate excellent production and functional molecule loading compared with hADSCs microspheres-EVs. The upregulation of eight miRNAs (i.e. hsa-miR-486-5p, hsa-miR-423-5p, hsa-miR-92a-3p, hsa-miR-122-5p, hsa-miR-223-3p, hsa-miR-320a, hsa-miR-126-3p, and hsa-miR-25-3p) and the downregulation of hsa-miR-146b-5p within hADSCs spheroids-EVs show the potential of improving the fate of remaining ear chondrocytes and promoting cartilage formation probably through integrated regulatory mechanisms. Additionally, a quick and innovative pipeline is developed for isolating chondrocyte homing peptide-modified EVs (CHP-EVs) from three-dimensional dynamic cultures of hADSCs spheroids. CHP-EVs are produced by genetically fusing a CHP at the N-terminus of the exosomal surface protein LAMP2B. The CHP + LAMP2B-transfected hADSCs spheroids were cultured with wave motion to promote the secretion of CHP-EVs. A harvesting method is used to enable the time-dependent collection of CHP-EVs. The pipeline is easy to set up and quick to use for the isolation of CHP-EVs. Compared with nontagged EVs, CHP-EVs penetrate the biomaterial scaffolds and specifically deliver the therapeutic miRNAs to the remaining ear chondrocytes. Functionally, CHP-EVs show a major effect on promoting cell proliferation, reducing cell apoptosis and enhancing cartilage formation in remaining ear chondrocytes in the M1 macrophage-infiltrated microenvironment.
    CONCLUSIONS: In summary, an innovative pipeline is developed to obtain CHP-EVs from three-dimensional dynamic culture of hADSCs spheroids. This pipeline can be customized to increase EVs production and functional molecule loading, which meets the requirements for regulating remaining ear chondrocyte fate in the M1 macrophage-infiltrated microenvironment.
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  • 文章类型: Journal Article
    背景:缺乏理想的填充材料是当前隆鼻的关键限制。通过自体软骨细胞再生软骨片有望提供理想的材料来源。然而,无法进行软骨片的微创移植极大地限制了这种材料的临床应用。在这篇文章中,作者提出了基于软骨片技术的可注射软骨微组织(ICM)的概念,目的是在临床实践中实现微创隆鼻。
    方法:从28名患者中收集约1.0cm2的耳后软骨。扩增分离的软骨细胞,然后通过高密度接种和在具有细胞因子的软骨形成培养基中的体外培养来构建自体软骨片(例如,转化生长因子β-1和胰岛素样生长因子-1)3周。接下来,ICM通过软骨片的颗粒化制备;然后将其注射到皮下口袋中用于隆鼻。
    结果:所有患者都成功准备了ICM,它的植入有效地提高了鼻背。磁共振成像证实注射部位存在再生组织;组织学检查显示成熟的软骨形成,具有典型的软骨空洞和丰富的软骨特异性细胞外基质沉积。在5年的随访中,83.3%的患者获得了优异或良好的术后患者满意度结果。只有两名患者(8.3%)明显吸收移植物。
    结论:这些结果表明,ICM可以促进人体内稳定的软骨再生和长期维持;ICM的植入使鼻背凹陷自然增强。
    方法:治疗,IV.
    BACKGROUND: A lack of ideal filling materials is a critical limitation in current rhinoplasty. Cartilage sheet regeneration by autologous chondrocytes is expected to provide an ideal source of material. However, the inability to perform minimally invasive transplantation of cartilage sheets has greatly limited the clinical application of this material. In this article, the authors propose the concept of injectable cartilage microtissue (ICM) based on cartilage sheet technology, with the aim of achieving minimally invasive augmentation rhinoplasty in clinical practice.
    METHODS: Approximately 1.0 cm2 of posterior auricular cartilage was collected from 28 patients. Isolated chondrocytes were expanded, then used to construct autologous cartilage sheets by high-density seeding and in vitro culture in chondrogenic medium with cytokines (eg, transforming growth factor beta-1 and insulin-like growth factor-1) for 3 weeks. Next, ICM was prepared by granulation of the cartilage sheets; it was then injected into a subcutaneous pocket for rhinoplasty.
    RESULTS: ICM was successfully prepared in all patients, and its implantation efficiently raised the nasal dorsum. Magnetic resonance imaging confirmed that regenerative tissue was present at the injection site; histologic examinations demonstrated mature cartilage formation with typical cartilage lacunae and abundant cartilage-specific deposition of extracellular matrix. Excellent or good postoperative patient satisfaction results were achieved in 83.3% of patients over 5 years of follow-up. Obvious absorption of grafts occurred in only two patients (8.3%).
    CONCLUSIONS: These results demonstrated that ICM could facilitate stable cartilage regeneration and long-term maintenance in the human body; the implantation of ICM enabled natural augmentation of the depressed nasal dorsum.
    METHODS: Therapeutic, IV.
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  • 文章类型: Journal Article
    背景:目前再生颞下颌关节(TMJ)关节软骨缺损的临床方法仅治疗症状(即疼痛和功能障碍),而不寻求恢复关节完整性以长期缓解。因此,我们研究了一种新型的自组装组织工程软骨,以克服TMJ再生的重要临床问题。
    目的:使用耳廓软骨细胞检查动态自我再生软骨(dSRC)的成熟,并评估一种新型的组合方法,包括点阵激光治疗和dSRC植入用于TMJ软骨修复。
    方法:在连续往复运动下培养107个新鲜收获的兔耳软骨细胞的悬浮液,以形成dSRC。培养2、4和8周后,dSRC样品用H&E染色,Safranin-O和甲苯胺蓝。对I型和II型胶原进行免疫组织化学(IHC)。使用分数铒激光在六个新收获的髁中产生通道(300-500μm直径和1.2-1.5mm深度)。测试了两组:激光消融病变中的dSRC(实验)和空的激光消融通道(对照)。将TMJ髁培养长达8周,并如上所述进行分析。
    结果:H&E染色显示与天然软骨相比dSRC中的高细胞密度。所有dSRC组表现出强烈的Safranin-O染色,表明高糖胺聚糖(GAG)产量和强烈的甲苯胺蓝染色显示高蛋白聚糖含量。IHC证实dSRC主要由II型胶原组成。与空通道相比,实验组在两个时间点显示出改善的软骨修复。
    结论:体外证明了dSRC活力和成功的基质形成。点阵激光消融和dSRC植入的结合增强了软骨修复。
    BACKGROUND: Current clinical approaches to regenerate temporomandibular joint (TMJ) articulating cartilage defects only treat the symptoms (i.e. pain and dysfunction) and do not seek to restore joint integrity for long-term relief. Therefore, we investigated a novel self-assembling tissue-engineered cartilage to overcome this significant clinical issue for TMJ regenerative purposes.
    OBJECTIVE: Examine the maturation of dynamic self-regenerating cartilage (dSRC) using auricular chondrocytes and evaluate a novel combinatorial approach with fractional laser treatment and dSRC implantation for TMJ cartilage repair.
    METHODS: A suspension of 107 freshly harvested rabbit ear chondrocytes was cultured under a continuous reciprocating motion to form the dSRC. After 2, 4 and 8 weeks of culture, dSRC samples were stained with H&E, Safranin-O and Toluidine Blue. Immunohistochemistry (IHC) was performed for collagens type I and II. Channels (300-500 μm diameter and 1.2-1.5 mm depth) were created in six freshly harvested condyles using a fractional Erbium laser. Two groups were tested: dSRC in a laser-ablated lesion (experimental) and an empty laser-ablated channel (control). TMJ condyles were cultured for up to 8 weeks and analysed as described above.
    RESULTS: H&E staining showed a high cell density in dSRC compared to native cartilage. All dSRC groups demonstrated intense Safranin-O staining, indicating high glycosaminoglycan (GAG) production and intense Toluidine Blue staining showed high proteoglycan content. IHC confirmed that dSRC consisted predominantly of collagen type II. The experimental group showed improved cartilage repair at both time points compared to the empty channels.
    CONCLUSIONS: dSRC viability and successful matrix formation were demonstrated in vitro. The combination of fractional laser ablation and dSRC implantation enhanced cartilage repair.
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  • 文章类型: Case Reports
    在10岁的雄性博洛尼亚犬中,怀疑原因不明的耳廓软骨炎,有五个月的双侧结节性疼痛性和溃疡性脓性肉芽肿性皮炎的病史,并有推定的耳廓软骨破坏。用免疫抑制剂量的泼尼松龙解决疼痛和病变,然而,这种情况导致耳廓和外部运河畸形。
    Auricular chondritis of unknown cause was suspected in a 10-year-old male Bolognese dog with a five-month history of painful bilateral nodular and ulcerative pyogranulomatous dermatitis of the pinnae with putative auricular cartilage destruction. Pain and lesions resolved with immunosuppressive doses of prednisolone, yet the condition resulted in deformity of both pinnae and external canals.
    怀疑一只10岁的雄性波伦亚犬患有不明原因的耳廓软骨炎,该犬有5个月的双侧耳廓结节性和溃疡性脓性肉芽肿性皮炎病史,并假定耳廓软骨破坏。使用免疫抑制剂量的泼尼松缓解疼痛和病变,但病因导致耳廓和外耳道畸形。.
    Une chondrite auriculaire d’étiologie inconnue est suspectée chez un bichon bolonais mâle de 10 ans qui présente depuis 5 mois une dermatite pyogranulomateuse nodulaire et ulcéreuse bilatérale douloureuse du pavillon de l\'oreille avec une destruction présumée du cartilage auriculaire. La douleur et les lésions disparaissent avec des doses immunosuppressives de prednisolone, mais l\'affection entraîne une déformation des deux pavillons et des conduits auriculaires externes.
    Bei einem 10 Jahre alten männlichen Bologneser mit einer 5 Monate lang andauernden Anamnese einer schmerzhaften bilateralen nodulären und ulzerativen pyogranulomatösen Dermatitis der Pinnae mit vermeintlicher aurikulärer Knorpeldestruktion unbekannter Ursache wurde eine aurikuläre Chondritis vermutet. Die Schmerzen und die Veränderungen verschwanden mit immunsuppressiven Dosen von Prednisolon, aber die Ätiologie verursachte dennoch eine Deformierung beider Pinnae und der äußeren Gehörkanäle.
    耳介軟骨の破壊を伴う有痛性の両側結節性および潰瘍性肉芽腫性皮膚炎を5ヵ月間認めた10歳の雄のボロニーズ犬において、原因不明の耳介軟骨炎が疑われた。痛みや病変は免疫抑制量のプレドニゾロン投与で消失したが、病因は両側耳介および外耳道の変形であった。.
    Suspeitou‐se de condrite auricular de causa desconhecida em um cão macho Bolonhês de 10 anos de idade com um histórico de cinco meses de dermatite piogranulomatosa ulcerativa e nodular bilateral no pavilhão auricular com suposta destruição de cartilagem auricular. A dor e as lesões resolveram com doses imunossupressoras de prednisolona apesar de a etiologia ter resultado na deformidade de ambas as orelhas e condutos auditivos.
    Se sospechó la existencia de una condritis auricular de causa desconocida en un perro boloñés de 10 años con historia de 5 meses de duración de una dermatitis nodular ulcerativa piogramulomatosa y bilateral en las orejas con posible destrucción del cartílago auricular. El dolor y las lesiones se resolvieron con dosis inmunosupresoras de prednisolona pero la enfermedad produjo deformación de ambas orejas y de los canales auriculares externos.
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  • 文章类型: Journal Article
    背景:缺乏鼻尖突起是亚洲鼻部常见的畸形。各种常用的鼻尖移植物需要解剖中隔软骨膜,它们中的大多数是具有非整合设计的自体软骨。一种蛇形膨体聚四氟乙烯(ePTFE)鼻尖移植物,稳定的尖端移植物,无需任何额外的组装和拼接,符合亚洲人的鼻部解剖特征。
    方法:回顾性研究2015-2022年北京大学第三医院接受鼻尖隆鼻的亚洲患者。鼻尖移植物分为三组:蛇形ePTFE结合牙甲软骨(n=15),只有肋软骨(n=25),只有耳甲软骨(n=17)。如果患者的鼻成形术不涉及上述任何移植物,则将其排除在外。视觉模拟量表,FACE-Q机头,FACE-Q鼻孔,鼻塞症状评价量表,术前、术后结果评价量表。
    结果:53例(93.0%)鼻背低,46例(80.7%)鼻短。三组间并发症发生率差异无统计学意义。术前、术后量表评分三组间差异有统计学意义(p<0.05)。分数改进,包括所有的尺度,肋软骨组最高,耳甲软骨组最低。
    结论:蛇形ePTFE鼻尖移植物可以是一种有效的综合替代品,与传统的自体植入物(牙甲和肋软骨)相比,它提供了长期的安全性和有效性。
    BACKGROUND: Lacking a nasal tip projection is a common deformity of Asian nasals. Various commonly used nasal tip grafts require dissecting septal perichondrium, most of them are autologous cartilage with a nonintegrated design. A snake-shaped expanded polytetrafluoroethylene (ePTFE) nasal tip graft is an integrated, stable tip graft without any additional assembly and splicing, conforming to the nasal anatomy characteristics of Asians.
    METHODS: A retrospective study was performed on Asian patients who underwent rhinoplasty in the nasal tip at Peking University Third Hospital from 2015 to 2022. Nasal tip grafts were categorized into three groups: snake-shaped ePTFE combined with conchal cartilage (n = 15), only costal cartilage (n = 25), and only conchal cartilage (n = 17). Patients were excluded if their rhinoplasty did not involve any of the grafts above. Visual Analogue Scale, FACE-Q Nose, FACE-Q Nostril, Nasal Obstruction Symptom Evaluation scale, and Rhinoplasty Outcome Evaluation scale were used to evaluate the preoperative and postoperative results.
    RESULTS: Fifty-three (93.0%) cases had low nasal dorsum and 46 (80.7%) cases had short nose. There was no significant difference in complication rates among the three groups. The difference between preoperative and postoperative scale scores was statistically significant among the three groups (p < 0.05). Score improvements, including all scales, were the highest in the costal cartilage group and lowest in the conchal cartilage group.
    CONCLUSIONS: Snake-shaped ePTFE nasal tip grafts can be an effective integrated alternative that provides long-term safety and efficacy compared with traditional autogenous implants (conchal and costal cartilages).
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  • 文章类型: Journal Article
    背景:作为一种罕见的耳廓畸形,尽管在过去的研究中描述了许多纠正中度至重度问号耳朵的外科手术,仍然需要探索一种更具成本效益的方法。耳软骨和周围皮肤的最佳利用同时实现优异的结果继续构成重大挑战。
    方法:从2018年到2023年,本研究纳入了24例单侧问号耳患者。其中7例为严重型畸形(耳廓下部缺失),和十七个是中度的(只有螺旋和小叶之间的裂隙)。所有患者均采用局部软骨和皮瓣的新方法治疗,未受累区域无损伤。
    结果:所有患者对问号耳显着改善和整体对称外观均满意。手术瘢痕不明显。未观察到并发症。随访期显示,纠正程序一直产生对称和美观的结果。
    结论:我们的新方法能够优化利用变形组织和周围皮肤,该方法对于校正中度至重度问号耳朵是有效和可靠的。
    方法:本期刊要求作者为每篇文章分配一定程度的证据。对于这些循证医学评级的完整描述,请参阅目录或在线作者说明www。springer.com/00266.
    BACKGROUND: As a rare auricular deformity, despite numerous surgical procedures for correcting moderate-to-severe question mark ears described in past studies, there remains a need to explore a more cost-effective approach. The optimal utilization of ear cartilage and surrounding skin while achieving superior outcomes continues to pose a significant challenge.
    METHODS: From 2018 to 2023, twenty-four patients with unilateral question mark ear were enrolled in this study. Seven of them were severe type deformities (absence of lower part of auricle), and seventeen were moderate (only cleft between helix and lobule). All patients were treated with new method using local cartilage and flap without damage in unaffected area.
    RESULTS: All patients were satisfied with significant improvement of question mark ear and the overall symmetrical appearance. The surgical scar was not obvious. No complications were observed. The follow-up period revealed that the corrective procedure kept producing the symmetrical and cosmetic results.
    CONCLUSIONS: Our new method enables optimal utilization of deformed tissue and surrounding skin, rendering this method effective and reliable for correcting moderate-to-severe question mark ears.
    METHODS: This journal requires that authors assign a level of evidence to each article. For a full description of these Evidence-Based Medicine ratings, please refer to the Table of Contents or the online Instructions to Authors www.springer.com/00266 .
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  • 文章类型: Journal Article
    小耳畸形是一种发病率较高的先天性耳廓发育不良,组织工程技术为耳廓的重建提供了一种有前途的策略。我们先前描述了由微耳软骨细胞构建的工程软骨表现出较差的生化和生物力学特性,这被认为是由于微耳软骨细胞的迁移能力降低所致。在目前的研究中,我们发现RhoGTPase成员在小耳软骨细胞中缺乏。通过过度表达RhoA,Rac1和CDC42,分别我们进一步证明,RhoA对小耳软骨细胞的迁移能力降低负有重要责任。此外,我们构建了基于PGA/PLA支架的软骨,以验证RhoA过表达的微小软骨细胞的软骨形成能力,结果表明,过表达RhoA对提高微耳软骨细胞工程软骨质量的帮助有限。然而,ADSCs的共培养显著改善了工程软骨的生化和生物力学特性。尤其是,共培养RhoA过表达的小耳软骨细胞和ADSCs对湿重产生了极好的影响,软骨特异性细胞外基质和工程软骨的生物力学特性。此外,我们提出了RhoA过表达的小耳软骨细胞和ADSCs的共培养,结合人耳形PGA/PLA支架和通过CAD/CAM和3D打印技术制造的钛合金支架,有效地构建和维持了体内耳廓结构。总的来说,我们的结果为RhoA在微小软骨细胞中的重要作用提供了证据,并为构建患者特异性组织工程耳廓软骨提供了开发策略.
    Microtia is a congenital auricle dysplasia with a high incidence and tissue engineering technology provides a promising strategy to reconstruct auricles. We previously described that the engineered cartilage constructed from microtia chondrocytes exhibited inferior levels of biochemical and biomechanical properties, which was proposed to be resulted of the decreased migration ability of microtia chondrocytes. In the current study, we found that Rho GTPase members were deficient in microtia chondrocytes. By overexpressing RhoA, Rac1, and CDC42, respectively, we further demonstrated that RhoA took great responsibility for the decreased migration ability of microtia chondrocytes. Moreover, we constructed PGA/PLA scaffold-based cartilages to verify the chondrogenic ability of RhoA overexpressed microtia chondrocytes, and the results showed that overexpressing RhoA was of limited help in improving the quality of microtia chondrocyte engineered cartilage. However, coculture of adipose-derived stem cells (ADSCs) significantly improved the biochemical and biomechanical properties of engineered cartilage. Especially, coculture of RhoA overexpressed microtia chondrocytes and ADSCs produced an excellent effect on the wet weight, cartilage-specific extracellular matrix, and biomechanical property of engineered cartilage. Furthermore, we presented that coculture of RhoA overexpressed microtia chondrocytes and ADSCs combined with human ear-shaped PGA/PLA scaffold and titanium alloy stent fabricated by CAD/CAM and 3D printing technology effectively constructed and maintained auricle structure in vivo. Collectively, our results provide evidence for the essential role of RhoA in microtia chondrocytes and a developed strategy for the construction of patient-specific tissue-engineered auricular cartilage.
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