psoriatic disease

  • 文章类型: Journal Article
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  • 文章类型: Journal Article
    循环滤泡辅助性T细胞(cTfh)和循环外周辅助性T细胞(cTph)(其与cTfh群体具有共同特征)与免疫介导的和自身免疫性疾病如银屑病(Ps)的发病机理有关。它们与白细胞介素17(IL-17)轴的紧密相互作用以及用于治疗Ps的靶向IL-17的生物制剂的离体作用难以捉摸。这项研究旨在研究靶向IL-17的生物制剂对从P患者血液中分离的cTfh和cTph细胞亚群的影响。
    在治疗开始和三个月后,从P患者中分离出外周血单核细胞(PBMC)。还从对照收集样品。使用单克隆抗体对细胞进行染色。流式细胞术评估cTfh(CD3+CD4+CXCR5+)和cTph(CD3+CD4+CXCR5-PD-1hi)细胞的分数。.
    流式细胞术分析显示,包括ICOS+和ICOS+PD-1+表达细胞的活化cTfh亚群分数增加,与对照组相比,患者。IL-17A的生物阻断减少了cTfh群体。此外,ICOS+和ICOS+PD-1+亚群也被抑制。最后,cTph细胞分数在生物制剂成功治疗3个月后显著下降.
    早期抗IL-17介导的Ps临床缓解与cTfh和cTph细胞亚群减少相关。
    UNASSIGNED: Circulating T follicular helper (cTfh) cells and circulating T peripheral helper (cTph) cells (which share common characteristics with the cTfh population) are implicated in the pathogenesis of immune-mediated and autoimmune diseases such as psoriasis (Ps). Their close interplay with the interleukin 17 (IL-17) axis and the ex vivo effect of IL-17-targeting biologic agents used to treat Ps on them are elusive. This study aimed to investigate the effect of biologics targeting IL-17 on cTfh and cTph cell subpopulations isolated from the blood of patients with Ps.
    UNASSIGNED: Peripheral blood mononuclear cells (PBMCs) were isolated from patients with Ps at treatment initiation and three months later. Samples were also collected from controls. Cells were stained using monoclonal antibodies. Flow cytometry assessed the fraction of cTfh (CD3+CD4+CXCR5+) and cTph (CD3+CD4+CXCR5-PD-1hi) cells..
    UNASSIGNED: Flow cytometric analysis showed increased fractions of activated cTfh subsets including ICOS+ and ICOS+PD-1+ expressing cells, in patients compared to controls. Biologic blocking of IL-17A diminished the cTfh population. Furthermore, ICOS+ and ICOS+PD-1+ sub-populations were also inhibited. Finally, the cTph cell fraction significantly decreased after three months of successful treatment with biologics.
    UNASSIGNED: Early anti-IL-17-mediated clinical remission in Ps is associated with decreased cTfh and cTph cell subpopulations.
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  • 文章类型: Journal Article
    关于COVID-19疫苗在银屑病和银屑病关节炎(银屑病疾病(PsD))患者中的有效性的信息有限。我们研究的目的是评估2020年12月至2021年12月,在PsD患者队列中,COVID-19mRNA疫苗在预防SARS-CoV-2阳性和严重感染中的有效性,以及免疫抑制剂与SARS-CoV-2感染相关结局的关系。在匹配的巢式病例对照研究中,使用根据人口统计学调整的条件逻辑回归评估疫苗有效性。合并症和免疫抑制剂的使用。研究结果包括SARS-CoV-2阳性和严重COVID-19(中度至重度COVID-19相关的住院或死亡)。至少一剂COVID-19mRNA疫苗与SARS-CoV-2阳性和严重COVID-19的风险降低相关(OR=0.41(95%CI,0.38-0.43)和OR=0.15(95%CI,0.11-0.20),分别)。与未接受任何疫苗的患者相比,接受三种疫苗剂量的患者的效果更为显着(OR(对于SARS-CoV-2阳性)=0.13(95%CI,0.12-0.15)和OR(对于严重疾病)=0.02(0.01-0.05))。依那西普和甲氨蝶呤与SARS-CoV-2阳性的高风险相关(1.58(1.19-2.10),p=0.001和1.25(1.03-1.51),分别为p=0.03)。总之,我们的结果表明,mRNACOVID-19疫苗可有效降低感染和严重的COVID-19相关结局.
    Limited information is available on the effectiveness of COVID-19 vaccination in patients with psoriasis and psoriatic arthritis (psoriatic disease (PsD)). The objective of our research was to assess the effectiveness of mRNA COVID-19 vaccination in preventing SARS-CoV-2 positivity and severe infection in a cohort of patients with PsD and the association of immunosuppressants on SARS-CoV-2 infection-related outcomes from December 2020 to December 2021. Vaccine effectiveness was assessed in a matched nested case control study using conditional logistic regression adjusted for demographics, comorbidities and immunosuppressant use. Study outcomes included SARS-CoV-2 positivity and severe COVID-19 (moderate-to-severe COVID-19-related hospitalizations or death). At least one dose of mRNA COVID-19 vaccine was associated with reduced risk of SARS-CoV-2 positivity and severe COVID-19 (OR = 0.41 (95% CI, 0.38-0.43) and OR = 0.15 (95% CI, 0.11-0.20), respectively). A more significant effect was found among patients who received three vaccines doses compared with those who did not receive any (OR (for positive SARS-CoV-2) = 0.13 (95% CI, 0.12-0.15) and OR (for severe disease) = 0.02 (0.01-0.05)). Etanercept and methotrexate were associated with higher risk of SARS-CoV-2 positivity (1.58 (1.19-2.10), p = 0.001 and 1.25 (1.03-1.51), p = 0.03, respectively). In conclusion, our results show that mRNA COVID-19 vaccines are effective in reducing both infection and severe COVID-19-related outcomes.
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  • 文章类型: Journal Article
    牛皮癣是一种炎症性皮肤病,在某些情况下伴有全身性表现。鉴于临床表现的多样性,银屑病这一术语可能更好地反映了这些患者的临床表现.
    在大多数情况下,皮肤病变先于关节受累,以及其他可能受累的器官,如肠和眼睛。各种免疫介导的细胞途径,如TNFα,IL-23、IL-17以及其他细胞因子参与银屑病疾病的病理生理学。
    对它们干扰我们免疫系统的方式的更好理解导致了疾病控制和结果的显着改善。这篇综述旨在强调银屑病疾病的最新治疗方法。预计将显著减少未满足的需求和治疗差距。
    UNASSIGNED: Psoriasis is an inflammatory skin disease that in some cases is accompanied by systemic manifestations. Given the varied clinical manifestations, the term psoriatic disease probably better reflects the clinical picture of these patients.
    UNASSIGNED: In most cases, the skin lesions precede joint involvement as well as other potentially involved organs such as the intestine and the eye. Various immune-mediated cellular pathways such as that of TNFα, IL-23, IL-17 as well as other cytokines are involved in the pathophysiology of the psoriatic disease.
    UNASSIGNED: A better understanding of the way they interfere with our immune system has led to remarkably better disease control and outcomes. This review aims to highlight the newest treatments for psoriatic disease, which are expected to significantly reduce unmet needs and treatment gaps.
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  • 文章类型: Journal Article
    银屑病(PsD),包括斑块型银屑病(PsO)和银屑病关节炎(PsA),包括广泛的表现,并显着影响生活质量(QoL)。这里,我们评估了患者对PsO和PsA作为全身性疾病的理解,它对他们的身体和情感健康的影响,和患者与医疗保健专业人员的经验,以分享治疗决策。
    全球牛皮癣病及其他疾病调查是一项横断面调查,定性,对伴有/不伴有PsA的中重度PsO患者进行的在线调查。此分析报告了印度患者的发现。
    在接受调查的261名患者中,27%与PsO报告伴随PsA,其中89%报告PsA严重程度为中度或高度活跃。总的来说,92%的人听说过“PsD”这个词,90%的人知道他们的病情是全身性疾病。很少有人知道PsD表现(掌足底银屑病,49%;指甲牛皮癣,43%;轴性症状,40%;PSA,34%)和合并症(心血管疾病,33%;肥胖,30%;糖尿病,28%)。89%的患者表示他们的皮肤问题对QoL有“非常大”到“极端大”的影响。97%的患者经历了他人的歧视和污名化。81%的患者没有参与确定治疗目标。很少(PsO,6%;PsA,9%)的患者对目前的治疗不满意;≥50%的患者报告皮肤症状(PsO)和关节症状(PsA)的不完全缓解是不满意的原因。
    对与PsD和QoL差相关的表现和合并症缺乏认识突出了对患者进行教育的必要性,共同的治疗决策,以及印度PsD管理的多维方法。
    UNASSIGNED: Psoriatic disease (PsD), including plaque psoriasis (PsO) and psoriatic arthritis (PsA), comprises a wide spectrum of manifestations and significantly impacts quality-of-life (QoL). Here, we assessed patients\' understanding of PsO and PsA as a systemic disease, its impact on their physical and emotional well-being, and patients\' experiences with healthcare professionals for shared treatment decision-making.
    UNASSIGNED: The Global Psoriatic Disease and Beyond Survey was a cross-sectional, qualitative, online survey conducted on patients with moderate-to-severe PsO with/without concomitant PsA. This analysis reports findings from Indian patients.
    UNASSIGNED: Of the 261 surveyed patients, 27% with PsO reported concomitant PsA, of whom 89% reported PsA severity as moderately or highly active. Overall, 92% had heard the term \"PsD,\" and 90% knew their condition was a systemic disease. Few were aware of PsD manifestations (palmoplantar psoriasis, 49%; nail psoriasis, 43%; axial symptoms, 40%; PsA, 34%) and comorbidities (cardiovascular disease, 33%; obesity, 30%; diabetes, 28%). Eighty-nine percent of patients indicated their skin problems had a \"very-large\" to \"extreme-large\" impact on QoL. Ninety-seven percent of patients experienced discrimination and stigmatization from others. Eighty-one percent of patients were not involved in deciding treatment goals. Few (PsO, 6%; PsA, 9%) patients were dissatisfied with current treatment; ≥50% patients reported incomplete relief of skin symptoms (PsO) and joint symptoms (PsA) as the reason for dissatisfaction.
    UNASSIGNED: Lack of awareness of the manifestations and comorbidities associated with PsD and poor QoL highlights the need for patient education, shared treatment decision-making, and a multidimensional approach to PsD management in India.
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  • 文章类型: Journal Article
    银屑病关节炎(PsA)是一种异质性,对患者生活质量产生负面影响的慢性炎症性疾病。患者报告的结果指标(PROM)用于在疾病评估中捕获患者观点,医生使用Psoriatic关节炎疾病活动指数(DAPSA)评估PsA的疾病活动。该研究旨在评估PsA影响的连续门诊患者的PROM与DAPSA评分之间的关系。
    一项横断面研究于2018年3月至2020年10月在意大利巴勒莫的ARNASCivico的PsA诊所进行,纳入门诊PsA患者。根据DAPSA评分评估患者的疾病活动性,和PROMs,如PHQ-9、HAQ、FACIT-F,和PsAID,进行了评估。线性回归分析评估了DAPSA评分与所包括的PROM之间的关系。
    158PsA连续的外周子集银屑病关节炎门诊患者。中位患病年限为10.6(9.3-11.9),中位DAPSA评分为19.02(9-33.1).回归分析强调了DAPSA评分和PsAID之间的强关系(adjR226%,p<0.0001),FACIT-F(adjR225.4%,p<0.0001),HAQ(adjR223.7%,p<0.0001),和PHQ-9(adjR215%,p<0.0001)。
    PROM与DAPSA评分密切相关,但它可以深入评估疾病对PsA患者不同生活领域的影响。
    UNASSIGNED: Psoriatic arthritis (PsA) is a heterogeneous, chronic inflammatory disease that negatively impacts patients\' quality of life. Patient-reported outcome measures (PROMs) are used to capture patient perspectives in disease assessment, and physicians use the Disease Activity Index for Psoriatic Arthritis (DAPSA) to evaluate disease activity in PsA. The study aimed to assess the relationship between PROMs and the DAPSA score in consecutive outpatients affected by PsA.
    UNASSIGNED: A cross-sectional study was conducted from March 2018 to October 2020 at the PsA clinic of the ARNAS Civico in Palermo (Italy), enrolling outpatients with PsA. Patients were assessed for their disease activity according to the DAPSA score, and PROMs, such as PHQ-9, HAQ, FACIT-F, and PsAID, were evaluated. Linear regression analysis evaluated the relationship between the DAPSA Score and the included PROMs.
    UNASSIGNED: 158 PsA consecutive peripheral subset psoriatic arthritis outpatients were recruited. The median years of illness was 10.6 (9.3-11.9), and the median DAPSA score was 19.02 (9-33.1). The regression analysis highlighted a strong relationship between the DAPSA score and the PsAID (adjR2 26%, p < 0.0001), the FACIT-F (adjR2 25.4%, p < 0.0001), the HAQ (adjR2 23.7%, p < 0.0001), and PHQ-9 (adjR2 15%, p < 0.0001).
    UNASSIGNED: PROMs are strongly associated with the DAPSA score, but it allows in-depth evaluation of the impact of the disease on different domains of PsA patients\' life.
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  • 文章类型: Review
    牛皮癣是一种炎症性皮肤病,在美国和加拿大影响了800多万人。大约,四分之一的银屑病患者患有炎性关节炎,称为银屑病关节炎(PsA)。包括银屑病和PsA的银屑病疾病被认为是一种免疫介导的炎性疾病。表现出自身免疫和自身炎症特征。介绍了有关银屑病疾病中自身抗体的存在和临床意义的最新文献。银屑病和PsA患者中几种自身抗体的频率及其对疾病诊断的临床意义,回顾了疾病活动和治疗反应。此外,介绍了抗体测定的基本原理,并分析了每项研究使用的方法。尽管历史上被描述为类风湿因子阴性(血清阴性)疾病,已在银屑病患者中鉴定出一系列自身抗体。这表明自身免疫成分可能在银屑病疾病中起作用;然而,需要更多的证据来确定这些自身抗体的临床效用.
    Psoriasis is an inflammatory skin disease affecting over 8 million people in the US and Canada. Approximately, a quarter of psoriasis patients have an inflammatory arthritis termed psoriatic arthritis (PsA). Psoriatic disease encompassing both psoriasis and PsA is regarded as an immune-mediated inflammatory disease, exhibiting both autoimmune and autoinflammatory features. A review of the current literature on the presence and clinical significance of autoantibodies found in psoriatic disease are presented. The frequency of several autoantibodies in psoriasis and PsA patients as well as their clinical significance regarding disease diagnosis, disease activity and treatment response are reviewed. Additionally, the basic principles of antibody assays are presented, and the methods used for each study are analyzed. Despite historically described as a rheumatoid factor negative (seronegative) disease, an array of autoantibodies has been identified in patients with psoriatic disease. This points to an autoimmune component potentially playing a role in psoriatic disease; however, additional evidence is needed to determine the clinical utility of these autoantibodies.
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  • 文章类型: Journal Article
    大约25%的银屑病患者患有称为银屑病关节炎(PsA)的炎性关节炎。人们对使用代谢组学等新技术识别和验证能够准确可靠地预测从牛皮癣到PsA的转化的生物标志物有强烈的兴趣。脂质,特别是,在银屑病疾病中具有重要意义。我们试图开发一种液相色谱-质谱(LC-MS)方法,该方法可与固相微萃取(SPME)结合使用,以分析脂肪酸和类似分子。在两个LC柱上测试了基于已发表的脂质研究的总共25种色谱方法。作为概念的证明,使用SPME处理牛皮癣病患者(n=27牛皮癣和n=26PsA)的血清样品,并在选定的LC-MS方法上运行。优化了分析脂肪酸和脂肪酸样分子的最佳方法,并将其应用于血清样品。使用多变量和单变量方法,在牛皮癣和PsA组之间,共有18个初步注释的分类为脂肪酸和其他脂质化合物的特征具有统计学意义。开发和优化的SPME-LC-MS方法能够检测脂肪酸和类似的脂质,这可能有助于区分牛皮癣和PsA患者。
    Approximately 25% of psoriasis patients have an inflammatory arthritis termed psoriatic arthritis (PsA). There is strong interest in identifying and validating biomarkers that can accurately and reliably predict conversion from psoriasis to PsA using novel technologies such as metabolomics. Lipids, in particular, are of key interest in psoriatic disease. We sought to develop a liquid chromatography-mass spectrometry (LC-MS) method to be used in conjunction with solid-phase microextraction (SPME) for analyzing fatty acids and similar molecules. A total of 25 chromatographic methods based on published lipid studies were tested on two LC columns. As a proof of concept, serum samples from psoriatic disease patients (n = 27 psoriasis and n = 26 PsA) were processed using SPME and run on the selected LC-MS method. The method that was best for analyzing fatty acids and fatty acid-like molecules was optimized and applied to serum samples. A total of 18 tentatively annotated features classified as fatty acids and other lipid compounds were statistically significant between psoriasis and PsA groups using both multivariate and univariate approaches. The SPME-LC-MS method developed and optimized was capable of detecting fatty acids and similar lipids that may aid in differentiating psoriasis and PsA patients.
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  • 文章类型: Journal Article
    基于有关银屑病(PSO)和银屑病关节炎(PSA)发生的致病步骤的知识的进步,已经逐步提出了银屑病疾病连续体的概念。评估生物分子(炎性细胞因子,炎性趋化因子,幼稚PSO患者的细胞粘附和细胞介质),带PSO的PSA,和PSA正弦PSO。考虑到牛皮癣指甲受累的存在,对结果进行分层,广泛的皮肤病和肥胖评估所有涉及的患者。
    通过多路复用技术,20血清生物分子被评估与促炎细胞因子(GM-CSF,IFN-γ,IL-1α,IL-1β,IL-6,IL-8,IL-12p70,IL-17A,IL-23,TNF),抗炎细胞因子(IFN-α,IL-4,IL-10,IL-13),炎性趋化因子(IP-10,MCP-1,MIP-1α,MIP-1β),细胞粘附和细胞介质(ICAM-1,E-选择素,P-选择素)。通过单向ANOVA评估三组的均值之间可能的统计学差异。此外,通过非参数T检验,我们根据选定的临床特征(银屑病指甲受累,PASI≥10,BMI≥30)。
    在80名未评估的患者中,与其他组相比,PSO患者E-选择素(p=0.021)和IL-8(0.041)显著升高.在患有PSO的PSA患者中,ICAM-1水平显著高于其他组(p=0.009).我们没有观察到比较促炎和抗炎细胞因子的进一步差异,炎性趋化因子,以及PSO患者的细胞粘附和细胞介质,带PSO的PSA,和PSA正弦PSO。银屑病甲癣患者的ICAM-1(p=0.010)和IP-10(0.030)水平显着升高。在PASI≥10的患者中,IL-8值显着增强(p=0.004),TNF(p=0.013),E-选择素(p=0.004),MIP-1α(p=0.003),和MIP-1β(p=0.039)。在BMI≥30的患者中,E-选择素的水平明显高于其他患者(p=0.035)。
    我们的发现可能表明,类似的细胞因子谱可能是PSO患者的特征,带PSO的PSA,和PSA正弦PSO,加强银屑病疾病连续体的概念。然而,也可能显示出一些差异,潜在的致病差异,并导致这些患者的临床异质性。
    The idea of psoriatic disease continuum has been progressively prompted based on the advances of the knowledge about the pathogenic steps underpinning the occurrence of psoriasis (PSO) and psoriatic arthritis (PSA). To evaluate biomolecules (inflammatory cytokines, inflammatory chemokines, cell adhesion and cellular mediators) in naïve patients with PSO, PSA with PSO, and PSA sine PSO. To stratify the results considering the presence of psoriatic nail involvement, extensive skin disease and obesity evaluating all involved patients.
    By multiplex technology, 20 serum biomolecules were assessed with the inclusion of pro-inflammatory cytokines (GM-CSF, IFN-γ, IL-1α, IL-1β, IL-6, IL-8, IL-12p70, IL-17A, IL-23, TNF), anti-inflammatory cytokines (IFN-α, IL-4, IL-10, IL-13), inflammatory chemokines (IP-10, MCP-1, MIP-1α, MIP-1β), cell adhesion and cellular mediators (ICAM-1, E-selectin, P-selectin). The assessment of possible statistical differences between the means of the three groups was performed by One-Way ANOVA. In addition, by non-parametric T-tests, we stratified the results according to selected clinical characteristics (psoriatic nail involvement, PASI ≥ 10, BMI ≥ 30).
    In 80 assessed naïve patients, patients with PSO showed significant increases of E-selectin (p=0.021) and IL-8 (0.041) than other groups. In patients with PSA with PSO, significant higher levels of ICAM-1 were observed (p=0.009) than other groups. We did not observe further differences comparing pro-inflammatory and anti-inflammatory cytokines, inflammatory chemokines, and cell adhesion and cellular mediators in patients with PSO, PSA with PSO, and PSA sine PSO. Patients with psoriatic onychopathy showed significant increased levels of ICAM-1 (p=0.010) and IP-10 (0.030) than others. In patients with PASI ≥ 10, significantly enhanced values of IL-8 (p=0.004), TNF (p=0.013), E-selectin (p=0.004), MIP-1α (p=0.003), and MIP-1β (p=0.039). In patients with BMI ≥ 30, significantly higher levels of E-selectin were pointed out (p=0.035) than others.
    Our findings may suggest that a similar cytokine profile may characterize naïve patients with PSO, PSA with PSO, and PSA sine PSO, reinforcing the concept of psoriatic disease continuum. However, some differences may be also shown, underlying possible pathogenic differences and leading to the clinical heterogeneity of these patients.
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