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趨化激素及其受體在台灣異位性皮膚炎疾病中之角色探討

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趨化激素及其受體在台灣異位性皮膚炎疾病中之角色探討

Roles of chemokines and chemokine receptors among

patients with atopic dermatitis in Taiwan

中文摘要

異位性皮膚炎是一種慢性反覆的發炎性皮膚疾病,病患通常搔癢難耐,並且在特

定部位有濕疹樣變化,患者個人或家族常有異位性體質(Atopy)。CC 趨化激素

是具有促發炎能力的分子,在異位性皮膚炎與過敏的病理機轉扮演重要角色。我

們利用

ELISA 來檢測病人組與對照組血漿中趨化激素的濃度,並使用流式細胞

儀來測量週邊血液單核球上趨化激素受體的表現量。實驗結果顯示病人組血漿中

的免疫球蛋白

E、RANTES、MIP-1 與 Eotaxin 的濃度較對照組高。病人組血

漿中的

MCP-1 較對照組低。趨化激素受器 CCR2、CCR3 與 CCR5 在兩組間表

現並無差異。此外,RANTES 啟動子區域的多型性對於 RANTES 的分泌量與異

位性皮膚炎盛行率的影響已被廣泛討論,之前的研究顯示在德國與匈牙利異位性

皮膚炎病童中

RNATES 啟動子的多型性與疾病有不同的相關性,因此我們利用

聚合脢連鎖反應與直接定序法來分析台灣地區異位性皮膚炎患者與對照組的

RANTES 啟動子區域的多型性。結果顯示,兩者之間的多型性表現並無差異。

綜合以上研究,

IgE 與 CC 趨化激素中的 RANTES、MIP-1、Eotaxin 在台灣地

區異位性皮膚炎患者體內的表現量確實有上升,而

RANTES 驅動子在-28 與

-403 位置產生的多型性與異位性皮膚炎並無相關。

英文摘要

Atopic dermatitis (AD) is a chronic, relapsing inflammatory skin disease

characterized by extreme pruritus, typically distributed eczematous skin lesions and a personal or family history of atopic diseases. CC chemokines are potent

proinflammatory molecules which play an important role in the pathophysiology of atopic dermatitis (AD) and allergy. We determined the plasma level of C-C

chemokines of AD and controls by ELISA and used flow cytometry to evaluate expression of chemokine receptors on peripheral blood mononuclear cells in both groups. Plasma levels of IgE, RANTES, MIP-1, and eotaxin were increased in severe AD patients, but not in moderate and mild AD compared with normal controls. MCP-1 level is lower in the patient group. Chemokine receptor CCR2, CCR3 and CCR5 were the same in both AD and control group. In addition, polymorphisms in promoter region of RANTES have been found, which increase the expression of these chemokines and affect the prevalence of atopic dermatitis. Different studies showed various roles of RANTES polymorphism in atopic dermatitis of German and Hungarian children. We also investigated whether the presence of these

(2)

polymorphisms was associated with atopic dermatitis in Taiwan. Atopic dermatitis patients and controls were screened for genotype with a PCR and direct sequencing- based assay. No significant difference in the frequency of the polymorphisms between atopic dermatitis patients and controls was found. Our finding suggests augmented production of some CC-chemokine such as RANTES, MIP-1, and eotaxin but no MCP-1 correlates with clinical severity of atopic dermatitis. In Taiwan population, there was no association between the -28G and -403A alleles polymorphism in the RANTES promoter and atopic dermatitis

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