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group_2_presentation_2_-_juvenile_arthritis [2017/03/08 16:45]
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group_2_presentation_2_-_juvenile_arthritis [2018/01/25 15:18] (current)
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 ===== Epidemiology ===== ===== Epidemiology =====
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-The incidence of JIA in North America and Europe ​ is 4 - 16 affected children out of a sub-population of 10000 children. 1 in 1000, or approximately 294000 children in the United States, are affected by the most common type of JIA in the United States, which is oligoarticular JIA. For reasons that continue to be studied, females seem to be affected with JIA more frequently than males. In the case of enthesitis-related JIA, males are affected more often than females. Furthermore,​ the incidence of JIA varies between different populations and ethnic groups (Genetics Home Reference, 2015). 
  
 <​sup>​[1]</​sup>​ <​sup>​[1]</​sup>​
 <box 60% round right |>​{{:​prev.png|{{:​epi_world_map.png|}}</​box| <box 60% round right |>​{{:​prev.png|{{:​epi_world_map.png|}}</​box|
 Figure 4.This image is showing the prevalence of the common forms of arthritis in the United States. Retrieved from: https://​rheumatoidarthritis.net/​wp-content/​uploads/​2013/​07/​prevalence_arthritis.png>​ Figure 4.This image is showing the prevalence of the common forms of arthritis in the United States. Retrieved from: https://​rheumatoidarthritis.net/​wp-content/​uploads/​2013/​07/​prevalence_arthritis.png>​
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 +The incidence of JIA in North America and Europe ​ is 4 - 16 affected children out of a sub-population of 10000 children. 1 in 1000, or approximately 294000 children in the United States, are affected by the most common type of JIA in the United States, which is oligoarticular JIA. For reasons that continue to be studied, females seem to be affected with JIA more frequently than males. In the case of enthesitis-related JIA, males are affected more often than females. Furthermore,​ the incidence of JIA varies between different populations and ethnic groups (Genetics Home Reference, 2015).
  
 In a study done by Saurenmann et al, questionnaires pertaining to ethnicity were distributed to patients with JIA and then followed up at the Hospital for Sick Children in Toronto. When the data was collected, the relative risk of developing JIA was calculated and the results were compared with data from the age matched general population in the Toronto region. The frequency at which JIA has been perceived shows that European descendants had about 69.7% of their patients diagnosed with JIA, which patients in the Toronto region has about 54.7%. Statistically lower percentages were shown to patients who were of the black, Asian, or Indian subcontinental origin. Kids from the European origin had a higher relative rate for developing any of the subtypes of juvenile arthritis, except oligoarthritis or psoriatic. Patients of the Asian origin showed to have a greater chance of being diagnosed with enthesitis-related JIA while those of black or Native North American origin were more likely to develop polyarticular rheumatoid positive JIA (Saurenmann,​ 2007).  ​ In a study done by Saurenmann et al, questionnaires pertaining to ethnicity were distributed to patients with JIA and then followed up at the Hospital for Sick Children in Toronto. When the data was collected, the relative risk of developing JIA was calculated and the results were compared with data from the age matched general population in the Toronto region. The frequency at which JIA has been perceived shows that European descendants had about 69.7% of their patients diagnosed with JIA, which patients in the Toronto region has about 54.7%. Statistically lower percentages were shown to patients who were of the black, Asian, or Indian subcontinental origin. Kids from the European origin had a higher relative rate for developing any of the subtypes of juvenile arthritis, except oligoarthritis or psoriatic. Patients of the Asian origin showed to have a greater chance of being diagnosed with enthesitis-related JIA while those of black or Native North American origin were more likely to develop polyarticular rheumatoid positive JIA (Saurenmann,​ 2007).  ​
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 Cytokines are protein messengers that transmit signals from one cell to another by binding to specific receptors on the surface of cells. Both pro- and anti-inflammatory cytokines, chemokines, and mitogenic factors are produced, but proinflammatory mediators predominate during the active phase of disease.Tumor necrosis factor alpha (TNFα)‎, IL-1, IL-6 and IL-17 are of key importance in the pathogenesis of inflammation in RA. IL-1 and TNFα‎ are also key players in the regulation of mediators of connective tissue damage by synoviocytes,​ including matrix metalloproteinases (MMPs) and prostaglandins (Nath Maini, 2010). Cytokines are protein messengers that transmit signals from one cell to another by binding to specific receptors on the surface of cells. Both pro- and anti-inflammatory cytokines, chemokines, and mitogenic factors are produced, but proinflammatory mediators predominate during the active phase of disease.Tumor necrosis factor alpha (TNFα)‎, IL-1, IL-6 and IL-17 are of key importance in the pathogenesis of inflammation in RA. IL-1 and TNFα‎ are also key players in the regulation of mediators of connective tissue damage by synoviocytes,​ including matrix metalloproteinases (MMPs) and prostaglandins (Nath Maini, 2010).
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 +<box 60% round right |>​{{:​p4.png|}}</​box|Figure 8: Summary of the pathogenic pathways in JIA. Retrived from: https://​www.researchgate.net/​profile/​Abdullah_Nahian/​publication/​263585727/​figure/​fig1/​AS:​202832654409738@1425370481906/​Figure-illustrates-the-pathogenic-pathways-of-rheumatoid-arthritis-following-31-38.png>​
  
 ACPAs may also bind to citrullinated proteins directly in the synovial membrane. Immune complexes between citrullinated proteins ,such as fibrinogen, and ACPA-igG can drive inflammation (including the production of IL-6 and tumor necrosis factor) by engaging both toll-like receptor (TLR4) and Fc receptors (Nath Maini, 2010). ACPAs may also bind to citrullinated proteins directly in the synovial membrane. Immune complexes between citrullinated proteins ,such as fibrinogen, and ACPA-igG can drive inflammation (including the production of IL-6 and tumor necrosis factor) by engaging both toll-like receptor (TLR4) and Fc receptors (Nath Maini, 2010).
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 Both ACPA- and RF-dependent events could contribute to the initiation and propagation of chronic synovial inflammation,​ and further synergize with T cell activation and enhance the local production of autoantibodies (McInnes & Schett, 2011). Both ACPA- and RF-dependent events could contribute to the initiation and propagation of chronic synovial inflammation,​ and further synergize with T cell activation and enhance the local production of autoantibodies (McInnes & Schett, 2011).
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-<box 60% round right |>​{{:​p4.png|}}</​box|Figure 8: Summary of the pathogenic pathways in JIA. Retrived from: https://​www.researchgate.net/​profile/​Abdullah_Nahian/​publication/​263585727/​figure/​fig1/​AS:​202832654409738@1425370481906/​Figure-illustrates-the-pathogenic-pathways-of-rheumatoid-arthritis-following-31-38.png>​ 
  
 ===Bone Destruction=== ===Bone Destruction===
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