puva

puva
  • 文章类型: Journal Article
    这篇文献综述探讨了特应性皮炎及其治疗,专注于光疗作为一种治疗方式。主要目的是阐明病理生理机制,临床表现,诊断标准,和特应性皮炎的流行病学。此外,它试图解释光疗机制,不同的模式,和其他治疗方法。在这次审查中,我们通过综合过去20年来自不同来源的发现来全面检查特应性皮炎。我们调查了流行病学,病理生理学,临床表现,诊断标准,以及光疗在治疗中的作用。我们进行主题分析,比较光疗方式,考虑上下文因素,并在坚持伦理考虑的同时整合患者的观点。局限性包括潜在的出版偏见,语言障碍,时间约束,主体性,和有限的泛化性。特应性皮炎具有复杂的发病机制,可以通过多种方式进行治疗。光疗作为一种有效和安全的治疗方法,特别是当其他疗法证明无效时。
    This literature review explores atopic dermatitis and its management, with a focus on phototherapy as a treatment modality. The primary objectives are to elucidate the pathophysiological mechanisms, clinical manifestations, diagnostic criteria, and epidemiology of atopic dermatitis. Additionally, it seeks to explain phototherapy mechanisms, different modalities, and other therapeutic approaches. In this review, we comprehensively examine atopic dermatitis by synthesizing findings from diverse sources over the past 20 years. We investigate the epidemiology, pathophysiology, clinical manifestations, diagnostic criteria, and role of phototherapy in treatment. We conduct thematic analysis, compare phototherapy modalities, consider contextual factors, and integrate patient perspectives while upholding ethical considerations. Limitations include potential publication bias, language barriers, temporal constraints, subjectivity, and limited generalizability. Atopic dermatitis has a complex pathogenesis and can be managed with diverse modalities. Phototherapy emerges as an effective and safe treatment, particularly when other therapies prove ineffective.
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  • 文章类型: Journal Article
    背景和目的斑秃(AA)是一种反复且无疤痕的脱发类型,可影响身体的任何毛状区域,尤其是头皮。它表现为斑驳或融合的脱发,人口统计学和种族不同。有许多治疗选择,包括局部和全身类固醇,局部米诺地尔,地物酚,他克莫司,补骨脂素和紫外线疗法(PUVA),接触免疫疗法,和口服免疫抑制药物。然而,在我们人群中,局部使用倍他米松与单独使用米诺地尔之间的疗效没有明显的对比.这项研究旨在比较局部使用二丙酸倍他米松与局部使用米诺地尔对AA患者的疗效。方法在皮肤科进行了一项非随机对照研究,拉合尔真纳医院,纳入2016年7月26日至2017年1月26日获得机构伦理批准后的患者数据.一百名脱发患者,无论是在头皮或任何其他毛茸茸的部分,来自两种性别,年龄在18至50岁之间,包括在研究中。创建了两个小组,患者根据临床医生的选择被分配到这些组.A组患者在患处每天两次施用二丙酸倍他米松(0.05%)洗剂,持续12周。B组患者在患处每天两次给予米诺地尔(5%)溶液,持续12周。随后进行了为期四周的随访计划。使用五点量表评分系统进行脱发分级。12周后,采用毛发再生评分(RGS)比较两组的疗效。结果共纳入100例S1~S3AA级病程小于3个月的患者。创建了两个小组,每组50名患者。A组平均年龄为29.08±6.51岁,而在B组中,29.38±6.62岁。A组,有76%的男性和24%的女性,而在B组中,有74%的男性和26%的女性。局部二丙酸倍他米松与局部米诺地尔在AA患者中的疗效比较显示,A组的疗效更高,为74%(3级和4级反应)。而在B组中,只有42%的患者显示出疗效。发现差异有统计学意义,P值为0.001。没有注意到严重的副作用。结论我们的研究得出的结论是,在AA患者中,与局部米诺地尔(5%)溶液相比,局部二丙酸倍他米松(0.05%)洗剂具有统计学上的更高疗效。
    Background and objective Alopecia areata (AA) is a reiterative and nonscarring type of hair loss that can affect any hairy area of the body, particularly the scalp. It manifests as patchy or confluent hair loss with variations in demographics and ethnicity. There are numerous treatment options available, including topical and systemic steroids, topical minoxidil, dithranol, tacrolimus, psoralen and ultraviolet therapy (PUVA), contact immunotherapy, and oral immunosuppressive drugs. However, no previous contrast for efficacy is present between the topical betamethasone versus topical minoxidil alone in our population. This study aims to compare the efficacy of topical betamethasone dipropionate versus topical minoxidil in patients with AA. Methodology A nonrandomized controlled study was conducted at the Department of Dermatology, Jinnah Hospital Lahore, incorporating the data of patients between July 26, 2016, and January 26, 2017, after obtaining institutional ethical approval. One hundred patients with alopecia, either on the scalp or any other hairy part, from both genders, aged between 18 and 50 years, were included in the study. Two groups were created, and patients were assigned to these groups based on the clinician\'s choice. Group A patients were administered betamethasone dipropionate (0.05%) lotion twice daily on affected areas for 12 weeks. Group B patients were administered minoxidil (5%) solution twice daily on affected areas for 12 weeks. A four-week follow-up plan was followed. A five-point scale score system was used for alopecia grading. After 12 weeks, the hair regrowth score (RGS) was used to compare the efficacy of treatment between the two groups. Results A total of 100 patients with grades S1 to S3 AA of less than three months duration were enrolled. Two groups were created, with 50 patients in each group. The mean age in Group A was 29.08 ± 6.51 years, while in Group B, it was 29.38 ± 6.62 years. In Group A, there were 76% males and 24% females, while in Group B, there were 74% males and 26% females. Comparison of efficacy of topical betamethasone dipropionate versus topical minoxidil in patients with AA demonstrated a greater efficacy of 74% (Grade 3 and Grade 4 responses) in Group A, while in Group B, only 42% of patients showed efficacy. A statistically significant difference was found, with a P-value of 0.001. No serious side effects were noted. Conclusions Our study concluded that topical betamethasone dipropionate (0.05%) lotion has statistically significantly higher efficacy compared to topical minoxidil (5%) solution in patients with AA.
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  • 文章类型: Journal Article
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  • 文章类型: Journal Article
    不同形式的光疗,是白癜风管理的支柱。结合治疗方式,如局部卡泊三醇(为了更快,更强烈的色素沉着),低剂量硫唑嘌呤与PUVA已被证明是有益的管理白癜风由于不同的色素沉着机制和它们的协同作用。局部应用bFGF相关的十肽(bFGFrP),然后进行阳光照射/UVA光疗,产生有效的再色素沉着。bFGFrP已显示出有助于较小病变的靶向光疗,并且其与其他治疗方式的组合非常有希望。然而,关于联合治疗的研究很少;特别是口服PUVA和bFGFrP。这项研究旨在评估bFGFrP与口服PUVA联合治疗白癜风(较大的体表面积20%或更多)的安全性和有效性。
    第四阶段,随机化,多中心研究(N=120)在6个月治疗期的成年稳定白癜风患者中,每月随访一次。补骨脂素(选项卡。Melanocyl)剂量0.6mg/kg,在暴露于UVA光疗前2小时口服。口服PUVA治疗,最初,在4J/cm2的照射剂量(PUVA组),如果耐受每周两次,则每四次增加0.5J/cm2。主要终点是靶病变的色素沉着(EOR)程度改善(最大尺寸至少2cm×2cm,没有白细胞增多),而次要终点是bFGFrP+口服PUVA联合治疗组和口服PUVA单药治疗组治疗期结束6个月时患者总体评估(PGA)和安全性的改善。
    6个月结束,61.8%(34例患者,n=55),而30.2%(16例患者,n=53)来自口服PUVA单一疗法组(n=53)。关于色素沉着(GOR)的等级,完全色素沉着为5.5%(3例,n=55)在联合治疗组,而单药治疗组(p≤0.05)没有患者表现出完全的色素沉着,联合组的PGA显示出显着的总体改善(p≤0.05);联合组的6例患者(10.9%)与1例(1.9%)显示出完全改善。治疗期间,没有报告不良事件.
    与口服PUVA单药治疗相比,口服PUVA治疗中添加bFGFrP导致强烈且更快地诱导色素沉着,具有良好的安全性。
    UNASSIGNED: Phototherapy in its different forms, is mainstay of vitiligo management. Combining treatment modalities like topical calcipotriol (for quicker, more intense repigmentation), Low dose azathioprine with PUVA have proven to be beneficial in management of vitiligo due to different mechanisms of repigmentation and their synergistic effects. Topical bFGF-related decapeptide (bFGFrP) application followed by sun exposure/ UVA phototherapy yields effective repigmentation. bFGFrP has shown to aid the targeted phototherapy in smaller lesions and its combinations with other treatment modalities have been very promising. However, there is paucity of studies on combination treatments; especially oral PUVA along with bFGFrP. This study was aimed at evaluating safety and efficacy of combination of bFGFrP with Oral PUVA in vitiligo (larger body surface area 20% or more).
    UNASSIGNED: Phase IV, randomized, multicentre study (N = 120) in adult patients with stable vitiligo of 6 months treatment period with monthly follow up visits. Psoralen (Tab. Melanocyl) dosage 0.6 mg/kg orally 2 h before exposure to UVA phototherapy. Oral PUVA therapy, initially, at an irradiation dose 4 J/cm2 (PUVA group), followed by increments 0.5 J/cm2 every four sittings if tolerated for twice weekly. Primary end point was improvement in extent of repigmentation (EOR) in target lesion (at least 2 cm × 2 cm in greatest dimension, without leukotrichia), while secondary endpoints were improvement in patient global assessment (PGA) and safety at end of 6 months of treatment period in bFGFrP + oral PUVA combination group and Oral PUVA monotherapy group.
    UNASSIGNED: End of 6 months, significantly greater EOR >50%) was achieved in 61.8% (34 patients, n = 55) from combination group while 30.2% (16 patients, n = 53) from the oral PUVA monotherapy group (n = 53). Regarding Grade of repigmentation (GOR), complete repigmentation was observed 5.5% (3 patients, n = 55) in combination group whereas no patient showed complete repigmentation in monotherapy group (p ≤ 0.05), PGA showed significant overall improvement in combination group (p ≤ 0.05); 6 patients (10.9%) from combination group Vs one (1.9%) showed complete improvement. During treatment period, there were no reported adverse events.
    UNASSIGNED: Addition of bFGFrP to oral PUVA therapy resulted in intense and faster induction of repigmentation than oral PUVA monotherapy with favorable safety profile.
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    文章类型: Journal Article
    在最近的几十年中,光疗在各种免疫介导的皮肤病的治疗中越来越受欢迎,因为与全身性治疗相比,光疗更具成本效益且毒性较小。本系统评价旨在告知皮肤科提供者光疗的风险和益处,尤其是有恶性肿瘤风险的患者。光疗产生的电离能量会导致DNA光沉积,即环丁烷嘧啶二聚体(CPD)和6-4光产物(6-4PP)。如果没有足够的维修,这些突变会增加致癌的风险。此外,光疗还可以通过形成活性氧(ROS)间接引起DNA损伤,其中一些结构和功能蛋白质和DNA的损伤。当选择光疗方式时,同样重要的是要考虑与每种模式相关的副作用。例如,与BB-UVB相比,需要高10倍剂量的NB-UVB来产生相似量的CPD。接受补骨脂素(PUVA)的UVA患者在接受最后一次治疗后25年内容易发生皮肤恶性肿瘤。根据每位患者的皮肤色素沉着水平和光适应潜力,提供者应该考虑最佳的辐射剂量。此外,已经提出了一些措施来尽量减少有害的皮肤变化,例如在UVB光疗和低频之前使用308nm准分子激光进行42摄氏度的热处理,低强度电磁场与UVB。然而,在进行常规皮肤检查时,在预防光疗诱导的瘤形成方面仍然至关重要。
    Phototherapy has gained popularity in the recent decades for the treatment of various immune-mediated dermatological conditions since it is more-cost effective and less toxic compared to systemic therapies. This systematic review aims to inform dermatology providers of the risks and benefits of phototherapy, especially in patients at risk for malignancies. Ionizing energy from phototherapy results in DNA photolesions, namely of cyclobutane pyrimidine dimers (CPDs) and 6-4 photoproducts (6-4PPs). Without adequate repair, these mutations increase the risk for carcinogenesis. Additionally, phototherapy can also indirectly cause DNA damage through the formation of reactive oxygen species (ROS), which damage of several structural and functional proteins and DNA. When choosing a phototherapy modality, it also important to take into consideration the side effect profiles associated with each modality. For instance, a 10-fold higher dose of NB-UVB is required to produce a similar amount of CPDs compared with BB-UVB. Patients who undergo UVA with psoralen (PUVA) can be susceptible to developing skin malignancies up to 25 years after receiving their last treatment. It would behoove providers to consider optimal radiation dosage given each patients\' level of skin pigmentation and potential for photoadaptation. Additionally, there are measures have been proposed to minimize deleterious skin changes, such as a 42-degree Celsius heat treatment using a 308nm excimer laser prior to UVB phototherapy and low frequency, low intensity electromagnetic fields along with UVB. However, as performing routine skin exams, remain paramount in the prevention of phototherapy-induced neoplasia.
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  • 文章类型: Journal Article
    未经证实:Morphea(局部硬皮病)是一种罕见的,慢性,炎性结缔组织疾病,以免疫系统功能障碍为特征,血管病变和皮肤纤维化。最有效的治疗方法之一是光疗。已发现光疗可通过诱导金属蛋白酶-1的表达有效治疗局部硬皮病。
    UNASSIGNED:比较补骨脂素和紫外线A(PUVA)和紫外线A1(UVA1)治疗前的金属蛋白酶(MMP-1)的浓度。
    UNASSIGNED:观察性研究是在一个研究中心进行的,包括接受PUVA和UVA1光疗治疗的广泛性硬伤患者。纳入研究的所有硬伤患者的平均年龄为55.7岁。通过ELISA(Biorbyt人MMP-1ELISA-酶联免疫吸附测定)检查MMP-1的水平。
    UASSIGNED:该研究表明,根据临床措施,接受PUVA和UVA1治疗的患者有所改善,导致临床评分降低。然而,治疗前后MMP-1浓度差异无统计学意义.局限性:研究样本相对较小。对更大的患者组的进一步研究将是有益的。
    UNASSIGNED:我们的数据表明,MMP-1浓度与光疗之间可能存在相关性。光疗治疗后发现MMP-1水平升高,这可能表明与患者对治疗的更好反应相关。然而,需要进一步的研究。
    UNASSIGNED: Morphea (localized scleroderma) is a rare, chronic, inflammatory connective tissue disease, characterized by immune system dysfunction, vasculopathy and skin fibrosis. One of the most effective treatments is phototherapy. Phototherapy has been found to be effective in treating localized scleroderma by inducing the expression of metalloproteinase-1.
    UNASSIGNED: To compare the concentrations of metalloproteinase (MMP-1) before psoralen and ultraviolet A (PUVA) and ultraviolet A1 (UVA1) treatments in the serum of patients with morphea.
    UNASSIGNED: The observational study was conducted in one research centre and included patients with generalised morphea who were treated with PUVA and UVA1 phototherapies. The mean age of all morphea patients included in the study was 55.7 years. The levels of MMP-1 were examined by ELISA (The Biorbyt Human MMP-1 ELISA - Enzyme-Linked Immunosorbent Assay).
    UNASSIGNED: The study showed that patients treated with PUVA and UVA1 had an improvement based on clinical measures, resulting in a reduction of clinical score. However, we did not observe statistically significant differences in MMP-1 concentrations before and after treatment. Limitations: The study sample was relatively small. Further studies on a larger group of patients would be beneficial.
    UNASSIGNED: Our data suggest that there is a possible correlation between MMP-1 concentrations and phototherapy. MMP-1 levels were found to be increased following phototherapy treatment, which may suggest a correlation with better response to treatment in patients with morphea. However, further research is needed.
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  • 文章类型: Journal Article
    白癜风是一种获得性皮肤色素沉着疾病,全球负担占人口的0.5%至2%。白癜风治疗经常会带来困难,这激发了人们对替代治疗方式的兴趣,包括多种维生素和草药补充剂。以前已经确定,营养在发展中起着至关重要的作用,放大,或修复一系列人类疾病。然而,饮食多样性与免疫介导的皮肤病之间的相关性仍有待解释。已经研究了几种补充剂,包括维生素,矿物,和草药补充剂。大多数研究认为,结合维生素B12,叶酸,阳光照射有利于诱导色素沉着。当与局部类固醇或UV-B(紫外线B)治疗结合使用时,锌和苯丙氨酸的补充由于它们在黑色素合成途径中的作用而对白癜风具有治疗作用。对草药补充剂进行的调查显示,其中大多数含有抗氧化剂,有助于色素沉着。这篇叙述性综述的目的是从最新和可靠的信息角度讨论营养在免疫介导的炎症性皮肤病中的作用。
    Vitiligo is an acquired skin pigmentation disease with a global burden of 0.5 to 2 percent of the population. Vitiligo therapy frequently poses a difficulty, which has sparked interest in alternative treatment modalities, including multivitamins and herbal supplementation. It has previously been established that nutrition plays a crucial role in developing, amplifying, or rehabilitating an array of human disorders. However, the correlation between diet diversity and immune-mediated skin diseases is still up to interpretation. Several supplements have been studied, including vitamins, minerals, and herbal supplements. Most studies agree that combining vitamin B12, folic acid, and sun exposure is good for inducing repigmentation. Supplementation of zinc and phenylalanine when used in conjunction with topical steroids or UV-B (ultraviolet B) treatment shows therapeutic effects on vitiligo due to their role in the melanin synthesis pathway. Investigations conducted on herbal supplements have revealed that most of them contain antioxidants, which aid in repigmentation. This narrative review\'s purpose is to discuss nutrition\'s function in immune-mediated inflammatory skin diseases from the perspective of the most recent and reliable information available.
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  • 文章类型: Journal Article
    在“光动力学基础”一节中,激光和PUVA治疗,“32份报告以全职和在线形式提交。各种科学学校的代表报告了在低强度红光照射和引入各种性质的光敏剂后在细胞和生物体水平上发生的过程的基础和应用研究的结果,其次是激光照射。科学报告提出了新的光敏剂,以及它们与生物活性分子的缀合物,用于肿瘤疾病的荧光诊断和光动力治疗。MikhailGrin教授提交了全体会议报告,“天然二氯是创造具有光诱导抗肿瘤和抗菌活性的药物的有希望的平台,“亚历山大·克拉斯诺夫斯基教授”在自然条件下激光激活溶解氧,\"和教授ElenaFilonenko\"光动力疗法在治疗面部皮肤的蠕动与局部应用基于5-ALA的凝胶。\"在海报区,年轻的科学家展示了18张海报,其中详细描述了部分报告中提出的研究。
    At the section \"Fundamentals of photodynamic, laser and PUVA therapy,\" 32 reports were presented in full-time and on-line format. Representatives of various scientific schools reported on the results of fundamental and applied research on the processes occurring at the cellular and organismal levels upon irradiation with low-intensity red light and upon the introduction of photosensitizers of various nature, followed by laser irradiation. Scientific reports proposed new photosensitizers, as well as their conjugates with biologically active molecules for fluorescent diagnostics and photodynamic therapy of oncological diseases. Plenary reports were presented by Professor Mikhail Grin \"Natural chlorins as a promising platform for creating drugs with photoinduced antitumor and antimicrobial activity,\" Professor Alexander Krasnovsky \"Laser activation of dissolved oxygen in natural conditions,\" and Professor Elena Filonenko \"Photodynamic therapy in the treatment of demodicosis of the facial skin with topical application of a gel based on 5-ALA.\" At the poster section, young scientists presented 18 posters, which describe in detail the research voiced in the section reports.
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  • 文章类型: Journal Article
    未经证实:Morphea(局部硬皮病)是一种炎性结缔组织疾病,以免疫系统功能障碍为特征,血管病变和皮肤纤维化。已发现光疗可有效治疗局部硬皮病。补骨脂素+紫外线A(PUVA)和紫外线A1(UVA1)光疗显着丰富的治疗可能性。
    UNASSIGNED:比较PUVA光化学疗法和UVA1光疗的临床效果,并评估治疗反应率。
    UNASSIGNED:这是一项回顾性的单中心研究和观察性研究,对所有接受PUVA和UVA光疗的硬伤患者进行了研究。我们回顾了2010年1月至2019年12月接受PUVA和UVA1光疗治疗的所有患者的光疗记录以及电子和纸质病例记录。
    UNASSIGNED:该研究表明,两组患者的临床指标均有所改善,导致所有组的临床评分降低。UVA1和PUVA光疗对硬伤患者有积极的短期和长期疗效。治疗反应率之间没有统计学差异。局限性:我们的研究样本相对较小,并且是回顾性研究,观察性研究。
    UNASSIGNED:我们的数据表明,紫外线PUVA和UVA1应考虑用于治疗播散性病变或对局部治疗无反应的硬叶。UVA1没有与口服补骨脂素相关的副作用,如恶心,呕吐,光角化病,但是我们表明,两者的有效性没有统计学优势。UVA1光疗是,然而,一种不太容易获得的治疗形式,提供更高质量的中心。
    UNASSIGNED: Morphea (localized scleroderma) is an inflammatory connective tissue disease, characterized by immune system dysfunction, vasculopathy and skin fibrosing. Phototherapy has been found to be effective in treating localized scleroderma. Psoralen + ultraviolet A (PUVA) and ultraviolet A1 (UVA1) phototherapy significantly enriched therapeutic possibilities.
    UNASSIGNED: To compare the clinical effect of PUVA photochemotherapy and UVA1 phototherapy and to evaluate the treatment response rates.
    UNASSIGNED: It was a retrospective one-centre research and observational study of all morphea patients treated with PUVA and UVA phototherapy. We reviewed phototherapy notes along with electronic and paper case records for all patients with morphea treated with PUVA and UVA1 phototherapy from January 2010 to December 2019.
    UNASSIGNED: The study shows that patients in both groups experienced improvement based on clinical measures, resulting in a reduction in the clinical score in all groups. There is positive short- and long-term efficacy of UVA1 and PUVA phototherapy in patients with morphea. There were no statistical differences between the treatment response rates. Limitations: We had a relatively small study sample and it was a retrospective, observational study.
    UNASSIGNED: Our data suggest that ultraviolet PUVA and UVA1 should be considered for the treatment of morphea with disseminated lesions or not responding to topical treatment. UVA1 is free of side effects linked to oral psoralens such as nausea, vomiting, photokeratosis, but we showed that there was no statistical advantage in the effectiveness of both. UVA1 phototherapy is, however, a less accessible form of treatment, available in the centres of higher quality.
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    文章类型: Journal Article
    光疗是中度至重度银屑病的标准治疗方法。然而,相关的皮肤致癌风险仍然令人担忧。我们的目标是对接受光疗的牛皮癣患者的皮肤癌风险进行系统评价。为了实现我们的目标,我们搜查了Cochrane,PubMed,和Embase数据库。我们旨在评估现有文献(从2010年7月1日至2020年12月31日)对所有Fitzpatrick皮肤光疗(FSP),其中包括71篇文章,和八篇文章被分类在这篇评论中。五项研究未报告窄带紫外线(UVB)和未指明的UVB对FSPII至VI的皮肤癌风险增加,一项研究未报告FSP。三项研究确实报告了窄带UVB和宽带UVB对FSPI-VI的皮肤癌风险增加,一项研究也没有指定皮肤光疗类型或UVB光疗类型。此外,一项使用补骨脂素和紫外线A伴和不伴窄带UVB的研究表明,在III型和IV型中,患皮肤癌的风险增加。光疗最常见的次要结果是光化性角化病(123)和日光性角化病(10)。许多患者还接受了额外的治疗,包括甲氨蝶呤,阿维酮,和生物制品。研究限制包括由于过去十年中关于该主题的研究数量有限而导致的发表偏倚以及报告的异质性。光疗之间的关系,牛皮癣,和皮肤致癌风险仍然矛盾。虽然牛皮癣的光疗是一种有效的治疗方法,需要进一步的研究来了解基于FSP的皮肤致癌风险,以帮助临床医师根据皮肤照型制定治疗建议.
    Phototherapy is a standard treatment for moderate-to-severe psoriasis. However, concern remains regarding the associated cutaneous carcinogenic risk. Our objective is to conduct a systematic review of skin cancer risk for psoriasis patients treated with phototherapy. To achieve our goal, we searched Cochrane, PubMed, and Embase databases. We aimed to evaluate existing literature (from July 1, 2010, to December 31, 2020) on phototherapy for all Fitzpatrick skin phototypes (FSP) which includes 71 articles, and eight articles being categorized in this review. Five studies did not report an increased skin cancer risk with narrowband-ultraviolet blue (UVB) and unspecified UVB for FSP II through VI, with one study not reporting FSP. Three studies did report an increased risk of skin cancer with narrowband-UVB and broadband-UVB for FSP I-VI, with one study also not specifying skin phototypes or UVB phototherapy type. Additionally, a study with psoralen and ultraviolet A with and without narrowband-UVB demonstrated an increased risk of skin cancer in phototypes III and IV. The most commonly reported secondary outcomes with phototherapy were actinic keratosis (123) and solar lentigines (10). Numerous patients were also on additional therapies including methotrexate, acitretin, and biologics. Study limitations include publication bias due to limited number of studies published on this topic in the last ten years along with heterogeneity in reporting. The relationship between phototherapy, psoriasis, and cutaneous oncogenic risk remains contradictory. While phototherapy for psoriasis is an efficacious therapy, further studies are needed to understand the cutaneous oncogenic risk based on FSP to help clinicals tailor treatment recommendations based on skin phototypes.
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