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Produção e caracterização funcional de uma nova evasina putativa de carrapatos Rhipicephalus microplus / Production and functional characterization of a novel putative evasin from Rhipicephalus microplus ticksNascimento, Mariana Oliveira 09 May 2019 (has links)
Carrapatos são parasitas hematófagos que secretam, em sua saliva, componentes imunomoduladores capazes de promover sua alimentação e suprimir as respostas imunológicas do hospedeiro. Dentre as classes de imunomoduladores presentes na saliva, encontram-se as evasinas, proteínas com capacidade de ligarem-se a quimiocinas, inibindo sua atividade relacionada ao recrutamento de células imunes. Neste trabalho, nós descrevemos a produção recombinante e caracterização estrutural e funcional de uma nova evasina putativa, a proteína Bm-nr-264079, identificada no sialotranscriptoma do carrapato bovino R. microplus. Observamos que a proteína Bm-nr-264079 apresenta similaridade estrutural com outras evasinas de carrapatos Rhipicephalus sanguineus já caracterizadas. A proteína foi produzida na forma recombinante com sucesso a partir da expressão em Escherichia coli Rosetta e purificação em condição desnaturante por cromatografia de afinidade a metais. Esta proteína apresentou atividade inibitória sobre o desenvolvimento de psoríase em modelo animal, limitando o desenvolvimento de lesão local nos animais tratados após a indução da doença por aplicação de imiquimode. A proteína Bm-nr- 264079 não apresentou efeito inibidor do crescimento de Staphylococcus aureus e Streptococcus uberis, bactérias que comumente colonizam a pele de bovinos suscetíveis à infestação por R. microplus. Os resultados aqui apresentados demonstram que a proteína Bm-nr-264079, em sua forma recombinante, apresenta atividade inibidora da inflamação, com potencial atividade de evasina. Novos estudos são necessários para uma caracterização mais específica das possíveis atividades farmacológicas desta proteína / Ticks are hematophagous parasites that secrete, in their saliva, immunomodulatory components capable of promoting their feeding and suppressing the immune responses of the host. Among the classes of immunomodulators present in saliva, we have the evasins, proteins capable of binding to chemokines, inhibiting the recruitment of immune cells. In this work, we describe the recombinant production and structural and functional characterization of a novel putative evasin, the protein Bm-nr-264079, identified in the sialotranscriptome of the R. microplus cattle tick. We have found that the protein Bm-nr-264079 shows structural similarity to other already characterized Rhipicephalus sanguineus tick evasins. The protein was successfully produced with expression in Escherichia coli Rosetta and purification in denaturing condition by metal affinity chromatography. This protein showed inhibitory activity on the development of psoriasis in the animal model, limiting the development of local lesion in the treated animals after the induction of the disease by the application of imiquimod. The protein Bm-nr-264079 showed no inhibitory effect on the growth of Staphylococcus aureus and Streptococcus uberis, bacteria that commonly colonize the skin of cattle susceptible to R. microplus infestations. The results presented herein demonstrate that Bm-nr-264079, in its recombinant form, exhibits antiinflammatory activity with potential evasin activity. Further studies are needed to characterize more specifically the pharmacological activities of this protein
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5-hydroxymethylcytosine is a key epigenetic regulator of keratinocyte stem cells during psoriasis pathogenesisYuan, Christine Wan-Yin 17 June 2019 (has links)
Epigenetic regulation is now known to play an important role in determining stem cell fate during normal tissue development and disease pathogenesis. In this study, we report loss of 5-hydroxymethylcytosine (5-hmC) mediated by ten-eleven translocation (TET) methylcytosine dioxygenases in keratinocyte stem cells (KSCs) and in their progenitor transit-amplifying (TA) cells of psoriatic lesions. We establish the DNA hydroxymethylation profile in both human psoriasis as well as in the imiquimod (IMQ)-induced mouse psoriasis model. Genome-wide mapping of 5-hmC in IMQ-treated mice epithelium revealed a loci-specific reduction of 5-hmC in genes associated with maintaining stem cell homeostasis including those involved in the RAR and Wnt/β-catenin signaling pathways. Restoration of TET expression in human KSC cultures via vitamin C treatment increased 5-hmC levels and induced more normal KSC differentiation. We found that by modulating 5-hmC levels in vitro, we could alter downstream expression of genes important in regulating stem cell homeostasis like nestin as well as IL-17R known to promote the psoriatic phenotype. Our findings demonstrate that loss of 5-hmC is a critical epigenomic phenomenon in KSCs and TA cells during psoriasis pathogenesis. / 2019-12-17T00:00:00Z
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Biomarkers of psoriatic arthritis phenotypesJadon, Deepak January 2016 (has links)
Background: Psoriatic arthritis (PsA) is a chronic heterogenous inflammatory arthritis with five phenotypes. The two least studied phenotypes are investigated in this thesis, including: psoriatic spondyloarthropathy (PsSpA) and psoriatic arthritis mutilans (PAM). The aims of this thesis were to determine the prevalence, clinical characteristics and radiographic characteristics of PsSpA and PAM in a cohort of PsA patients, and serum-soluble bone- turnover biomarkers of these phenotypes. Aims: Comparisons were made with PsA patients without axial disease (pPsA), and ankylosing spondylitis (AS) patients. Methods: A prospective single-centre cross-sectional study was conducted of PsA and AS patients. Serum on psoriasis-only patients (PsC) and healthy controls (HC) were also obtained. Multivariate clinical, radiographic, genetic and serum biomarker comparisons were made between these five groups of subjects. Results: The study enrolled 201 PsA and 201 AS patients, who were then reclassified as 118 PsSpA, 127 pPsA and 157 AS cases, alongside 200 PsC and 50 HC subjects. Several clinical biomarkers, imaging biomarkers, serum-soluble biomarkers and genetic biomarkers were identified that differentiate PsSpA from pPsA and AS. PsSpA affected a significant proportion of PsA patients, and was not a milder version of AS. PsSpA involvement was as disabling and clinically impactful as AS. PAM was found to be associated with PsSpA, and clinical biomarkers of PAM occurrence and radiographic progression were identified. Conclusions: In conclusion, this thesis indicates that PsSpA is on a spectrum of musculoskeletal disease, in between pPsA and AS; with PsSpA comprising a continuum itself, and with a phenotype expression related to disease duration. These findings may prompt the inception of an international-consensus classification system for PsSpA, for which there is a great clinical need. Given that PsSpA has its own discrete clinical and biomarker signature, its clinical management and research should be tailored from that of pPsA and AS. Ultimately this may further the effort for stratified and personalised medicine.
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Livskvalitet och lidande hos människor med psoriasisPerciwall, Michelle January 2008 (has links)
Psoriasis kan ha en stark påverkan på den hälsorelaterade livskvaliteten. Sjukdomen kan medföra hinder i psykiska och fysiska funktioner, hinder som är jämförbara med dem som ses vid cancer, ledinflammation, hypertoni, hjärtsjukdom, diabetes och depression. Det finns idag ingen behandling som helt botar psoriasis eller följdsjukdomen psoriasisartrit, i stället verkar den behandling som erbjuds främst symtomlindrande. Syftet med studien är att undersöka hur det är att leva med psoriasis och på vilket sätt sjukdomen kan medföra lidande. Metoden som används är litteraturstudier för att skapa en litteraturöversikt där likheter och skillnader mellan de ingående studiernas resultatdel undersöks. Resultatet visar att psoriasis har en kraftig påverkan på livskvaliteten och därmed medför olika former av lidande för de drabbade. Missnöjet kring behandlingarna är stort. Ett problem är att det finns lite tidigare forskning gjord kring psoriasis och livskvalitet med den kvalitativa ansatsen. Människor med psoriasis blir på grund av andra människors okunskap drabbade av missförstånd och inte minst nedvärderas allvaret i lidandet vid sjukdomen. Diskussionen visar att visst lidande, inte minst vårdlidandet, går att minska genom en ökad förståelse för hur det är att leva med psoriasis. Även attityden hos vårdpersonal behöver förändras. En ökad medvetenhet hos vårdare kan minska lidandet och öka den hälsorelaterade livskvaliteten. / <p>Program: Sjuksköterskeutbildning</p><p>Uppsatsnivå: C</p>
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銀屑病証治的古今文獻研究王俊杰, 01 January 2007 (has links)
No description available.
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A study of psoriasis : a methodological critiqueFord, Prudence Craig, Ford, Roberta Jeanne, Swanson, Susan 01 January 1979 (has links)
According to the National Psoriasis Foundation (1976), psoriasis is a little known and poorly understood skin disease afflicting an estimated eight million victims in the United States. About fifteen thousand new cases of psoriasis are diagnosed each year. It affects men and women in equal numbers at any age, most often between the ages of fifteen and thirty-five.
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The expression and molecular functions of LRIG proteins in cancer and psoriasis / Uttryck och molekylära funktioner av LRIG proteiner i cancer och psoriasisKarlsson, Terese January 2013 (has links)
The leucine-rich repeats and immunoglobulin-like domains (LRIG) family consists of three integral membrane proteins that are important in human cancer. LRIG1 is a negative regulator of growth factor signaling. Its expression is associated with longer survival in several cancer types, and the gene has been shown to function as a tumor suppressor. The roles of LRIG2 and LRIG3 are less well known. The aim of this thesis was to improve our understanding of the expression and function of the LRIG protein family in psoriasis and cancer. To investigate their expression in psoriasis, the mRNA levels and subcellular localization of the LRIG proteins were analyzed and compared between normal and psoriatic human skin. There were no differences in the LRIG mRNA levels between psoriatic and normal skin samples. However, the subcellular localization of all three LRIG proteins differed between psoriatic and normal skin. To study the physiological and molecular functions of Lrig2, we generated Lrig2E12-/- mice. These mice were viable and born at a Mendelian rate, but Lrig2E12-/- mice had an increased rate of spontaneous mortality and a transient reduction in growth rate compared to Lrig2 wild-type (wt) mice. In an orthotopic platelet-derived growth factor (PDGF)B-driven brain tumor mouse model, we studied the effect of Lrig2 on gliomagenesis. All Lrig2 wt mice developed tumors; 82% developed grade II/III tumors, and 18% developed grade IV tumors. Only 77% of the Lrig2E12-/- mice developed tumors, and they were all grade II/III tumors. Thus, Lrig2 increased the incidence and malignancy rates of PDGFB-driven gliomas. We then analyzed the effect of Lrig2 on Pdgf receptor (Pdgfr) signaling. Lrig2 had no effect on Pdgfr steady-state levels, the starvation-induced up-regulation of Pdgfrs, the phosphorylation of Pdgfrs, primary cilium formation or the PDGFBB-induced phosphorylation of Akt or Erk1/2. However, the kinetics of induction of the immediate-early genes Fos and Egr2 were altered, resulting in a more rapid induction in Lrig2E12-/- cells. We then analyzed the clinical and biological importance of LRIG1 in lung cancer. In a human lung cancer tissue micro-array (TMA), LRIG1 expression was found to be an independent positive prognostic factor for adenocarcinoma. To study the importance of Lrig1 regarding lung cancer development in vivo, we used an inducible EGFRL858R-driven mouse lung cancer model. The mice developed diffuse lung adenocarcinoma, and the tumor burden was greater in Lrig1-/- mice than in Lrig1+/+ mice (p = 0.025) at 60 days. The human lung cancer cell line H1975, with either normal or Tet-induced expression of LRIG1, was injected into the flanks of Balb/cA nude mice. Tumors formed by LRIG1-overexpressing cells were smaller than those formed by parental cells, further indicating that LRIG1 is important during lung tumor formation or growth. In vitro, LRIG1 suppressed the proliferation of H1975 cells and down-regulated the phosphorylation of MET and RET. To investigate the molecular functions of LRIG proteins further, we performed a yeast two-hybrid (YTH) screen using a peptide from the cytosolic tail of LRIG3 as bait. This screen identified LMO7 and LIMCH1 as prominent interaction partners for LRIG3. Proximity ligation assays showed that LMO7 interacted with all of the LRIG proteins at endogenous expression levels. LMO7 and LIMCH1 were expressed in all human tissues analyzed. Their expression was dramatically decreased in lung cancer compared to normal lung tissue. The expression of LMO7 was analyzed in a human lung cancer TMA. LMO7 was expressed in respiratory epithelial cells in normal lungs. However, LMO7 was only expressed in a quarter of the lung tumors. LMO7 expression was found to be an independent negative prognostic factor for lung cancer. In summary, we found that the LRIG proteins were redistributed in psoriatic skin. In a mouse glioma model, Lrig2 promoted oligodendroglioma genesis. LRIG1 was an independent positive prognostic factor in human lung cancer. Lrig1 ablation increased the tumor size in an EGFRL858R-driven lung cancer mouse model. LRIG1 expression decreased the tumor growth of human lung cancer cells in a xenograft mouse model. LMO7 interacted with all three LRIG proteins and was an independent negative prognostic factor in human lung cancer. These data demonstrate the importance of LRIG proteins in human disease.
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A novel role for activin in wound healing and psoriasis induction of a sensory neuropeptide /Cruise, Bethany Ann. January 2004 (has links)
Thesis (Ph. D.)--Case Western Reserve University, 2004. / [School of Medicine] Department of Neurosciences. Includes bibliographical references. Available online via OhioLINK's ETD Center.
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Genetic and Environmental Risk Factors for Psoriatic Arthritis among Patients with PsoriasisEder, Lihi 06 January 2012 (has links)
Aim: Most of the patients with Psoriatic Arthritis (PsA) develop arthritis following the onset of psoriasis. The aim of the project is to identify genetic and environmental risk factors for PsA among psoriasis patients.
Methods: PsA and psoriasis patients from two prospective cohorts were analyzed. The incidence of PsA among a prospective cohort of psoriasis patients was assessed. The distribution of Human Leukocyte Antigen (HLA) alleles and Killer Cell Immunoglobulin like Receptors (KIRs) and their combinations was compared between PsA, psoriasis and healthy controls. In addition, the association between a wide range of environmental exposures and PsA was evaluated by comparing the frequencies of exposed individuals among patients with recent onset PsA and psoriasis. The association between smoking and PsA was further investigated. The prevalence of smoking was in PsA, psoriasis and the general population. The interaction between HLA-C*06 and smoking was also tested.
Results: The genetic analysis revealed several HLA-B alleles and HLA haplotypes that are associated with PsA compared to psoriasis and can potentially serve as independent markers for PsA. Furthermore, several combinations of KIR genes and their respective HLA ligands were also found to be associated with PsA compared to psoriasis. The incidence of PsA among psoriasis patients was found to be higher than previously reported and its rate was constant over time. HLA-C*06 was associated with increased interval between psoriasis onset and PsA. Several environmental factors including occupational exposures, infections, injuries and smoking were associated with development of PsA. The prevalence of smoking was decreased among PsA patients compared to psoriasis. The interaction between HLA-C*06 and smoking was found to be significant.
Conclusions: Genetic and environmental factors are associated with the development of PsA in patients with psoriasis. These factors may serve as specific markers to identify psoriasis patients at increased risk for PsA.
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Genetic and Environmental Risk Factors for Psoriatic Arthritis among Patients with PsoriasisEder, Lihi 06 January 2012 (has links)
Aim: Most of the patients with Psoriatic Arthritis (PsA) develop arthritis following the onset of psoriasis. The aim of the project is to identify genetic and environmental risk factors for PsA among psoriasis patients.
Methods: PsA and psoriasis patients from two prospective cohorts were analyzed. The incidence of PsA among a prospective cohort of psoriasis patients was assessed. The distribution of Human Leukocyte Antigen (HLA) alleles and Killer Cell Immunoglobulin like Receptors (KIRs) and their combinations was compared between PsA, psoriasis and healthy controls. In addition, the association between a wide range of environmental exposures and PsA was evaluated by comparing the frequencies of exposed individuals among patients with recent onset PsA and psoriasis. The association between smoking and PsA was further investigated. The prevalence of smoking was in PsA, psoriasis and the general population. The interaction between HLA-C*06 and smoking was also tested.
Results: The genetic analysis revealed several HLA-B alleles and HLA haplotypes that are associated with PsA compared to psoriasis and can potentially serve as independent markers for PsA. Furthermore, several combinations of KIR genes and their respective HLA ligands were also found to be associated with PsA compared to psoriasis. The incidence of PsA among psoriasis patients was found to be higher than previously reported and its rate was constant over time. HLA-C*06 was associated with increased interval between psoriasis onset and PsA. Several environmental factors including occupational exposures, infections, injuries and smoking were associated with development of PsA. The prevalence of smoking was decreased among PsA patients compared to psoriasis. The interaction between HLA-C*06 and smoking was found to be significant.
Conclusions: Genetic and environmental factors are associated with the development of PsA in patients with psoriasis. These factors may serve as specific markers to identify psoriasis patients at increased risk for PsA.
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