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中文摘要  近十年來,

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透過Paralogs 概念建置的 SWOP 系統來找出疾病的路徑

中文摘要

近十年來, microarray 技術的進步,讓我們可以發現不同的基因在病理學上 或是生理學上表現不同;但是到目前為止仍然沒有證據可以證明他們之間的 關係。在這篇研究當中,我們發展了一個全新方法,透過 paralogs 的概念、

microarray 基因表現的資料、基因網路和 GO 的資料來找到疾病和正常路徑之 間交叉的基因。首先透過生物反應 (biological reaction) ,如白質交互作用 (pro tein-protein interactions) 、蛋白質調控 (protein-DNA regulations) 、磷酸化 (pho sphorylations) 和甲基化 (methylations) 把基因組 (genome) 連結成一個巨大的基 因網路。接下來根據每個基因在 GO 的特性把整個網路切成成千上萬條路徑

,也因為如此就可以把單獨的基因表現量換成路徑的表現量。最後搜尋疾病

和正常的路徑之間的 paralogous 基因,也許可能會在兩組之間找到相同的基

因,而這相同的基因可能和 paralogous 基因有關。在這套系統中,使用者可

以上傳人類、老鼠以及大鼠的 microarray 資料,透過系統的分析後所得到的

MI 就可以找到兩組有 paralogous 基因的兩組路徑,而且可以以圖形化的方式

呈現兩組路徑,而其中相同的基因則會特別的標示出來。 SWOP 系統透過 pa

ralogs 和複雜的 microarray 資料所找到疾病和正常路徑兩組之間相同基因,或

許可以拿來研究藥物所要抑制的基因。

(2)

Disease Pathway Finder Using Web-based SWOP (SideWays Observation via Paralogs) System by the Concept of Paralogs

英文摘要

From the viewpoint of evolution, gene duplication produces two functionally redundant, paralogous genes and thereby frees one of them from selective constraints. Divergent evolution has made tumor counterpart cells survived easier. Recently, microarray emerges as a nice approach to find distinct individual genes that differentially expressed between physiological and pathological cells, where, however, no clues to show th e relationship among these gene cluster. Here in the research, we developed a brand new approach that com bines the concept of paralogs, microarray gene expression data, gene network, gene ontology to obtain inte rsectional genes where the point that disease has gone astray from normal pathways. Firstly, we exerted the biological reactions, such as protein-protein interactions, protein-DNA regulations, phosphorylations, meth ylations, etc. to the genomes to build up network connectivity. Secondly, we partitioned the network into h undreds of thousands of pathways according to the GO cellular component properties of each gene, where helps to calculate the differentially expressed pathways rather than just differentially expressed genes. Fina lly, We searched for paralogous genes appeared in the contrary differentially pathways of normal and disea se status, respectively. It is very likely to find an intersectional gene between different pathways, because t his intersectional gene has higher probability to associate with both these paralogous genes in different situ ation.

Users are allowed to upload their microarray data of human, rat or mouse. The system would identify differ entially expressed pathways between normal and disease tissues by calculating with mutual information m ethods. The matched counterpart pathways that associated paired paralogs would be identified and visualiz ed in a graph. The intersectional genes would be therefore spotted and highlighted in the graph. This SWO P system facilitates to transform complex microarray data into simplified intersectional genes between dise ase and normal pathways by using the duplicate paralogs as which indicate the shortest evolutionary time where disease go wrong from normal pathways. In addition, it helps to design drug targets to inhibit the dis ease pathways.

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