韓劇電影你都看哪一部呢?論文書籍站
國立臺北科技大學 電資學院外國學生專班(iEECS) 白敦文所指導 VAIBHAV KUMAR SUNKARIA的 An Integrated Approach For Uncovering Novel DNA Methylation Biomarkers For Non-small Cell Lung Carcinoma (2022),提出Fujii Mina關鍵因素是什麼,來自於Lung Cancer、LUAD、LUSC、NSCLC、DNA methylation、Comorbidity Disease、Biomarkers、SCT、FOXD3、TRIM58、TAC1。
而第二篇論文國立臺北教育大學 體育學系碩士班 翁梓林所指導 何志俊的 著地失敗型態對膝外翻角度及膝外翻力矩之影響 (2021),提出因為有 動力學逆過程、額狀面生物力學、前十字韌帶、失衡的重點而找出了 Fujii Mina的解答。
Fujii Mina進入發燒排行的影片
#후지이미나 #구독자명 #이벤트
드디어 ‘톡! TALK! 후지이 미나’ 채널에도 구독자명이 생겼습니다😊
정말 많은 분들이 참여해주셔서 댓글 읽으면서 즐거웠어요.
이제 구독자명도 생겼으니 더 소통하는 채널 만들 수 있게 노력할게요^^
ついに「トーク!TALK!藤井美菜」チャンネルにも視聴者名が出来ました。
本当にたくさんの方々が参加してくださり、コメントを読みながら、楽しかったです^^
これからは視聴者名もついたので、もっと疎通するチャンネルになるように頑張ります^^
Finally, 'Toc! Talk! Fujii Mina' channel get a subscriber name.
I was happy because many subscriber participate to event while I read a your ideas.
Subscriber name is made so I try to communicate with you ^^
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An Integrated Approach For Uncovering Novel DNA Methylation Biomarkers For Non-small Cell Lung Carcinoma
為了解決Fujii Mina 的問題,作者VAIBHAV KUMAR SUNKARIA 這樣論述:
Introduction - Lung cancer is one of primal and ubiquitous cause of cancer related fatalities in the world. Leading cause of these fatalities is non-small cell lung cancer (NSCLC) with a proportion of 85%. The major subtypes of NSCLC are Lung Adenocarcinoma (LUAD) and Lung Small Cell Carcinoma (LUS
C). Early-stage surgical detection and removal of tumor offers a favorable prognosis and better survival rates. However, a major portion of 75% subjects have stage III/IV at the time of diagnosis and despite advanced major developments in oncology survival rates remain poor. Carcinogens produce wide
spread DNA methylation changes within cells. These changes are characterized by globally hyper or hypo methylated regions around CpG islands, many of these changes occur early in tumorigenesis and are highly prevalent across a tumor type.Structure - This research work took advantage of publicly avai
lable methylation profiling resources and relevant comorbidities for lung cancer patients extracted from meta-analysis of scientific review and journal available at PubMed and CNKI search which were combined systematically to explore effective DNA methylation markers for NSCLC. We also tried to iden
tify common CpG loci between Caucasian, Black and Asian racial groups for identifying ubiquitous candidate genes thoroughly. Statistical analysis and GO ontology were also conducted to explore associated novel biomarkers. These novel findings could facilitate design of accurate diagnostic panel for
practical clinical relevance.Methodology - DNA methylation profiles were extracted from TCGA for 418 LUAD and 370 LUSC tissue samples from patients compared with 32 and 42 non-malignant ones respectively. Standard pipeline was conducted to discover significant differentially methylated sites as prim
ary biomarkers. Secondary biomarkers were extracted by incorporating genes associated with comorbidities from meta-analysis of research articles. Concordant candidates were utilized for NSCLC relevant biomarker candidates. Gene ontology annotations were used to calculate gene-pair distance matrix fo
r all candidate biomarkers. Clustering algorithms were utilized to categorize candidate genes into different functional groups using the gene distance matrix. There were 35 CpG loci identified by comparing TCGA training cohort with GEO testing cohort from these functional groups, and 4 gene-based pa
nel was devised after finding highly discriminatory diagnostic panel through combinatorial validation of each functional cluster.Results – To evaluate the gene panel for NSCLC, the methylation levels of SCT(Secritin), FOXD3(Forkhead Box D3), TRIM58(Tripartite Motif Containing 58) and TAC1(Tachikinin
1) were tested. Individually each gene showed significant methylation difference between LUAD and LUSC training cohort. Combined 4-gene panel AUC, sensitivity/specificity were evaluated with 0.9596, 90.43%/100% in LUAD; 0.949, 86.95%/98.21% in LUSC TCGA training cohort; 0.94, 85.92%/97.37 in GEO 66
836; 0.91,89.17%/100% in GEO 83842 smokers; 0.948, 91.67%/100% in GEO83842 non-smokers independent testing cohort. Our study validates SCT, FOXD3, TRIM58 and TAC1 based gene panel has great potential in early recognition of NSCLC undetermined lung nodules. The findings can yield universally accurate
and robust markers facilitating early diagnosis and rapid severity examination.
著地失敗型態對膝外翻角度及膝外翻力矩之影響
為了解決Fujii Mina 的問題,作者何志俊 這樣論述:
背景:非接觸性前十字韌帶傷害通常發生於運動中的著地動作,膝外翻可能是導致前十字韌帶受傷的因子之一。許多研究將著地動作成功或失敗的試驗 (failed trail) 設定標準加以判斷之,通常會將失敗的試驗從分析中刪除。然而,著地期間失敗試驗中包含動力學和運動學參數,可能對非接觸性運動傷害的機制形成,提供一項很重要的線索。目的:探討足部滑動失衡、軀幹傾斜失衡、跳步失衡等三種著地失敗型態及著地成功對膝外翻角度及膝外翻力矩之影響。方法:以大學男性運動員共11名,且近半年並任何下肢運動傷害史及開刀病史。執行單腳側向著地動作,並以著地瞬間測力板訊號產生 ( >10 N) 至著地後1000毫秒定義為著地期
。以動力學逆過程方法計算膝外翻力矩及髖外展力矩。以單因子相依樣本變異數進行分析,顯著水準為 (α=.05) 。結果:在著地瞬間髖內收角度,著地成功組顯著小於跳步失衡組。著地期最大髖角度,軀幹側傾組顯著小於著地成功組、跳步失衡組與足部滑動組;在最大膝外翻角度,著地成功組顯著小於跳步失衡組、足部滑動組與軀幹側傾組;足部滑動組顯著大於著地成功組、跳步失衡組與軀幹側傾組。著地成功組在最大髖外展力矩顯著小於跳步失衡組。結論: 跳步失衡與軀幹側傾失衡因著地期髖內收角度與足部滑動失衡因著地期膝外翻角度之影響,而造成膝關節傷害風險相對提高,因此透過本研究發現在未來訓練與比賽現場,提供不同著地失敗型態科學訊息,
進而減少下肢運動傷害。