Imilar scores for the three predictors. (TIF) Figure S8 Kaplan-Meier overall survival stratification between COXEN-matched and unmatched buy APTO-253 patients in the TCGA-448 cohort. (A) all patients (B) RG7800MedChemExpress RG7800 platinum-sensitive patients, (C) platinum-resistant patients. (TIF) Figure S9 Kaplan-Meier progression-free survival stratification between COXEN-matched and unmatched patients in the TCGA-448 cohort. (A) all patients (B) platinum-sensitive patients, (C) platinum-resistant patients. (TIF) Figure S10 Kaplan-Meier overall survival stratification between COXEN-matched and unmatched patients in the recurrent EOC patients in TCGA-448 cohort. (A) all patients (B) platinum-sensitive patients, (C) platinum-resistant patients. (TIF) Methods S1 Supporting methods.Supporting InformationFigure SROC and AUC analysis of 3 final predictors (A) ROC analysis of paclitaxel prediction of 107 patients in Bonome cohort, (B) ROC of cyclophosphamide prediction of 68 patients in Bonome cohort, (C) ROC of topotecan prediction of 41 patients in TCGA-UW. (TIF)Figure S2 Kaplan-Meier survival analysis of predictedresponders and nonresponders among recurrent EOC patients treated with paclitaxel. (A) all patients, (B) platinumsensitive patients, (C) platinum-resistant patients. (TIF)Figure S3 Kaplan-Meier survival analysis of predictedresponders and nonresponders in independent patient cohorts. (A) paclitaxel predictor prediction for OS in UVA-51, (B) paclitaxel predictor prediction for PFS in UVA-51. (TIF)Figure S4 Kaplan-Meier survival analysis of predicted(DOCX)Results Sresponders and nonresponders among recurrent EOC patients treated with cyclophosphamide. (A) all patients, (B) platinum-sensitive patients, (C) platinum-resistant patients. (TIF)Figure S5 Kaplan-Meier survival analysis of predictedSupporting results.(ZIP)Author ContributionsConceived and designed the experiments: YK SRG SJL KB DT JRD JKL. Performed the experiments: YK JKL. Analyzed the data: YK JKL. Wrote the paper: YK SRG SJL KB DT JKL JRD.responders and nonresponders among recurrent EOC patients treated with topotecan (A) all patients, (B)
In 2011, UNAIDS estimated that more than 34 million people living with HIV, 1.7 m died from an AIDS related disease and 2.5 million became newly infected with HIV. The HIV/AIDS epidemic is continuing to grow; the number of those infected is increasing by more than 500,000 per annum [1]. Discovering how to prevent the transmission of HIV is of primary concern to health care authorities worldwide [2]. It is well known from a range of observational and epidemiological studies that the lifetime risk of acquiring HIV among males can be significantly reduced by approximately 60 through safe male circumcision (SMC). Numerous papers on the topic have been published over the past two decades to elevate HIV prevention awareness, especially in sub-Saharan countries [3,4,5].In 2009, the US Government (USAID) reported that scaling up male circumcision to reach 80 percent of adult males in 14 African countries by 2015 could potentially avert more than 4 million adult HIV infections between 2009 and 2025 and yield annual cost savings of US 1.4?.8 billion after 2015, with a total net savings of US 20.2 billion between 2009 and 2025 [6,7]. Today, there are over 38 million adolescent and adult males in East and southern Africa who could benefit from safe male circumcision for HIV prevention. The challenge Africa faces is how to safely scale up a surgical procedure in resource limited setting.Imilar scores for the three predictors. (TIF) Figure S8 Kaplan-Meier overall survival stratification between COXEN-matched and unmatched patients in the TCGA-448 cohort. (A) all patients (B) platinum-sensitive patients, (C) platinum-resistant patients. (TIF) Figure S9 Kaplan-Meier progression-free survival stratification between COXEN-matched and unmatched patients in the TCGA-448 cohort. (A) all patients (B) platinum-sensitive patients, (C) platinum-resistant patients. (TIF) Figure S10 Kaplan-Meier overall survival stratification between COXEN-matched and unmatched patients in the recurrent EOC patients in TCGA-448 cohort. (A) all patients (B) platinum-sensitive patients, (C) platinum-resistant patients. (TIF) Methods S1 Supporting methods.Supporting InformationFigure SROC and AUC analysis of 3 final predictors (A) ROC analysis of paclitaxel prediction of 107 patients in Bonome cohort, (B) ROC of cyclophosphamide prediction of 68 patients in Bonome cohort, (C) ROC of topotecan prediction of 41 patients in TCGA-UW. (TIF)Figure S2 Kaplan-Meier survival analysis of predictedresponders and nonresponders among recurrent EOC patients treated with paclitaxel. (A) all patients, (B) platinumsensitive patients, (C) platinum-resistant patients. (TIF)Figure S3 Kaplan-Meier survival analysis of predictedresponders and nonresponders in independent patient cohorts. (A) paclitaxel predictor prediction for OS in UVA-51, (B) paclitaxel predictor prediction for PFS in UVA-51. (TIF)Figure S4 Kaplan-Meier survival analysis of predicted(DOCX)Results Sresponders and nonresponders among recurrent EOC patients treated with cyclophosphamide. (A) all patients, (B) platinum-sensitive patients, (C) platinum-resistant patients. (TIF)Figure S5 Kaplan-Meier survival analysis of predictedSupporting results.(ZIP)Author ContributionsConceived and designed the experiments: YK SRG SJL KB DT JRD JKL. Performed the experiments: YK JKL. Analyzed the data: YK JKL. Wrote the paper: YK SRG SJL KB DT JKL JRD.responders and nonresponders among recurrent EOC patients treated with topotecan (A) all patients, (B)
In 2011, UNAIDS estimated that more than 34 million people living with HIV, 1.7 m died from an AIDS related disease and 2.5 million became newly infected with HIV. The HIV/AIDS epidemic is continuing to grow; the number of those infected is increasing by more than 500,000 per annum [1]. Discovering how to prevent the transmission of HIV is of primary concern to health care authorities worldwide [2]. It is well known from a range of observational and epidemiological studies that the lifetime risk of acquiring HIV among males can be significantly reduced by approximately 60 through safe male circumcision (SMC). Numerous papers on the topic have been published over the past two decades to elevate HIV prevention awareness, especially in sub-Saharan countries [3,4,5].In 2009, the US Government (USAID) reported that scaling up male circumcision to reach 80 percent of adult males in 14 African countries by 2015 could potentially avert more than 4 million adult HIV infections between 2009 and 2025 and yield annual cost savings of US 1.4?.8 billion after 2015, with a total net savings of US 20.2 billion between 2009 and 2025 [6,7]. Today, there are over 38 million adolescent and adult males in East and southern Africa who could benefit from safe male circumcision for HIV prevention. The challenge Africa faces is how to safely scale up a surgical procedure in resource limited setting.