Your search keyword '"Michael Shi"' showing total 66 results

1. On the numerical performance of finite-difference-based methods for derivative-free optimization

Author

Hao-Jun Michael Shi, Melody Qiming Xuan, Figen Oztoprak, and Jorge Nocedal

Subjects

Control and Optimization, Applied Mathematics, Software

Published

2022

2. Phase I study of MSB2311, a novel pH-dependent anti-PD-L1 monoclonal antibody, treating patients with advanced solid tumors and lymphoma

Author

Qi Zhang, Jian Zhang, Haijun Zhong, Ying Yuan, Lei Yang, Qingyuan Zhang, Dongmei Ji, Jifang Gong, Jing Li, Zhenling Yao, Chuan Qi, Jianming Wang, Lingmin Lu, Michael Shi, Xueming Qian, Lin Shen, Jian Li, and Xichun Hu

Subjects

Cancer Research, Oncology, Immunology, Immunology and Allergy

Published

2023

3. Data from Targeting FGFR with Dovitinib (TKI258): Preclinical and Clinical Data in Breast Cancer

Author

José Baselga, Alejandro Yovine, Diana Graus Porta, Andrea Kay, Yong Zhang, Michael Shi, Stephanie Deudon, John W. Smith, Hope Rugo, Nicholas Turner, Sara A. Hurvitz, Jose M. Perez-Garcia, Florence Dalenc, Mario Campone, Thomas Bachelot, and Fabrice André

Abstract

Purpose: Fibroblast growth factor receptor 1 (FGFR1) and FGFR2 amplifications are observed in approximately 10% of breast cancers and are related to poor outcomes. We evaluated whether dovitinib (TKI258), an inhibitor of FGFR1, FGFR2, and FGFR3, presented antitumor activity in FGFR-amplified breast cancers.Experimental Design: Preclinical activity of dovitinib was evaluated in both breast cancer cell lines and an FGFR1-amplified xenograft model (HBCx2). Dovitinib was then evaluated in a phase II trial that included 4 groups of patients with human EGF receptor 2–negative metastatic breast cancer on the basis of FGFR1 amplification and hormone receptor (HR) status. FGFR1 amplification was assessed by silver in situ hybridization. Preplanned retrospective analyses assessed predictive value of FGFR1, FGFR2, and FGF3 amplifications by quantitative PCR (qPCR).Results: Dovitinib monotherapy inhibits proliferation in FGFR1- and FGFR2-amplified, but not FGFR-normal, breast cancer cell lines. Dovitinib also inhibits tumor growth in FGFR1-amplified breast cancer xenografts. Eighty-one patients were enrolled in the trial. Unconfirmed response or stable disease for more than 6 months was observed in 5 (25%) and 1 (3%) patient(s) with FGFR1-amplified/HR-positive and FGFR1-nonamplified/HR-positive breast cancer. When qPCR-identified amplifications in FGFR1, FGFR2, or FGF3 were grouped to define an FGF pathway–amplified breast cancer in HR-positive patients, the mean reduction in target lesions was 21.1% compared with a 12.0% increase in patients who did not present with FGF pathway–amplified breast cancer.Conclusion: Dovitinib showed antitumor activity in FGFR-amplified breast cancer cell lines and may have activity in breast cancers with FGF pathway amplification. Clin Cancer Res; 19(13); 3693–702. ©2013 AACR.

Published

2023

4. Supplementary Figure 1 from Targeting FGFR with Dovitinib (TKI258): Preclinical and Clinical Data in Breast Cancer

Author

José Baselga, Alejandro Yovine, Diana Graus Porta, Andrea Kay, Yong Zhang, Michael Shi, Stephanie Deudon, John W. Smith, Hope Rugo, Nicholas Turner, Sara A. Hurvitz, Jose M. Perez-Garcia, Florence Dalenc, Mario Campone, Thomas Bachelot, and Fabrice André

Abstract

PDF file - 20K, Dovitinib effectively targets FGFR1 in vivo. FGF23 levels were measured from plasma taken at baseline and during dovitinib treatment in 18, 33, and 20 patients from the FGFR1+/HR+, FGFR1-/HR+, and FGFR1-/HR- patient groups, respectively. Error bars represent the 95% confidence intervals.

Published

2023

5. Supplementary Data from ASCEND-7: Efficacy and Safety of Ceritinib Treatment in Patients with ALK-Positive Non–Small Cell Lung Cancer Metastatic to the Brain and/or Leptomeninges

Author

Dong-Wan Kim, Michael Shi, Fabrice Branle, Yuanbo Song, Pilar Cazorla Arratia, Felipe K. Hurtado, Pilar Garrido, Chong-Jen Yu, Mark McKeage, Margarita Majem, Rita Chiari, Sergey Orlov, Chao-Hua Chiu, Patrick Y. Wen, Heather A. Wakelee, Martin J. van den Bent, Erin M. Bertino, Fabrice Barlesi, and Laura Q.M. Chow

Abstract

Supplementary Data from ASCEND-7: Efficacy and Safety of Ceritinib Treatment in Patients with ALK-Positive Non–Small Cell Lung Cancer Metastatic to the Brain and/or Leptomeninges

Published

2023

6. Supplementary Table 1 from Phase I Study of Dovitinib (TKI258), an Oral FGFR, VEGFR, and PDGFR Inhibitor, in Advanced or Metastatic Renal Cell Carcinoma

Author

Bernard Escudier, Andrea Kay, Michael Shi, Julie Chang, Paramita Sen, Jean-Charles Soria, Daniel Castellano, Andrea Harzstark, Jürgen E. Gschwend, Chia-Chi Lin, Jose A. Lopez-Martin, and Eric Angevin

Abstract

PDF file - 49K, Supplemental Table 1. Criteria for defining dose-limiting criteria

Published

2023

7. Supplementary Figure 1 from Phase II Results of Dovitinib (TKI258) in Patients with Metastatic Renal Cell Cancer

Author

Eric Angevin, Michael Shi, Matthew Squires, Nicoletta Pirotta, Sarah Beall, Andrea Harzstark, Jürgen E. Gschwend, Chia-Chi Lin, Daniel Castellano, Yen-Chuan Ou, Alain Ravaud, Viktor Grünwald, and Bernard Escudier

Abstract

PDF file - 57KB, Supplemental Figure 1 contains the longitudinal plot of model-adjusted fold change from baseline for plasma VEGF.

Published

2023

8. Supplementary Figure from ASCEND-7: Efficacy and Safety of Ceritinib Treatment in Patients with ALK-Positive Non–Small Cell Lung Cancer Metastatic to the Brain and/or Leptomeninges

Author

Dong-Wan Kim, Michael Shi, Fabrice Branle, Yuanbo Song, Pilar Cazorla Arratia, Felipe K. Hurtado, Pilar Garrido, Chong-Jen Yu, Mark McKeage, Margarita Majem, Rita Chiari, Sergey Orlov, Chao-Hua Chiu, Patrick Y. Wen, Heather A. Wakelee, Martin J. van den Bent, Erin M. Bertino, Fabrice Barlesi, and Laura Q.M. Chow

Abstract

Supplementary Figure from ASCEND-7: Efficacy and Safety of Ceritinib Treatment in Patients with ALK-Positive Non–Small Cell Lung Cancer Metastatic to the Brain and/or Leptomeninges

Published

2023

9. Supplementary Figure Legend, Table 1 from Targeting FGFR with Dovitinib (TKI258): Preclinical and Clinical Data in Breast Cancer

Author

José Baselga, Alejandro Yovine, Diana Graus Porta, Andrea Kay, Yong Zhang, Michael Shi, Stephanie Deudon, John W. Smith, Hope Rugo, Nicholas Turner, Sara A. Hurvitz, Jose M. Perez-Garcia, Florence Dalenc, Mario Campone, Thomas Bachelot, and Fabrice André

Abstract

PDF file - 61K, Growth Inhibition in FGFR1- and FGFR2-Amplified Cell Lines.

Published

2023

10. Data from Phase II Results of Dovitinib (TKI258) in Patients with Metastatic Renal Cell Cancer

Author

Eric Angevin, Michael Shi, Matthew Squires, Nicoletta Pirotta, Sarah Beall, Andrea Harzstark, Jürgen E. Gschwend, Chia-Chi Lin, Daniel Castellano, Yen-Chuan Ou, Alain Ravaud, Viktor Grünwald, and Bernard Escudier

Abstract

Purpose: Fibroblast growth factor (FGF) signaling regulates tumor growth and vascularization and partly mediates antiangiogenic escape from VEGF receptor (VEGFR) inhibitors. Dovitinib (TKI258) is a tyrosine kinase inhibitor (TKI) that inhibits FGF receptor (FGFR), VEGFR, and platelet-derived growth factor receptor, which are known drivers of antiangiogenic escape, angiogenesis, and tumor growth in renal cell carcinoma (RCC).Experimental Design: Patients with advanced or metastatic RCC were treated with oral dovitinib 500 mg/day (5-days-on/2-days-off schedule). The study population was enriched for patients previously treated with a VEGFR TKI and an mTOR inhibitor.Results: Of 67 patients enrolled, 55 patients (82.1%) were previously treated with ≥1 VEGFR TKI and ≥1 mTOR inhibitor (per-protocol efficacy set). The 8-week overall response rate and disease control rate in this population were 1.8% and 52.7%, respectively. Disease control rate during the entire study period was 56.4% (50.9% ≥4 months). Median progression-free survival and overall survival in the entire population were 3.7 and 11.8 months, respectively. Pharmacodynamic analyses demonstrated dovitinib-induced inhibition of VEGFR (as determined by increased levels of placental growth factor and decreased levels of soluble VEGFR2) and FGFR (as determined by increased FGF23 serum measures). The most frequently reported treatment-related adverse events of all grades included nausea (65.7%), diarrhea (62.7%), vomiting (61.2%), decreased appetite (47.8%), and fatigue (32.8%).Conclusion: Dovitinib was shown to be an effective and tolerable therapy for patients with metastatic RCC who had progressed following treatment with VEGFR TKIs and mTOR inhibitors. Clin Cancer Res; 20(11); 3012–22. ©2014 AACR.

Published

2023

11. Supplementary Figure Legend from Phase II Results of Dovitinib (TKI258) in Patients with Metastatic Renal Cell Cancer

Author

Eric Angevin, Michael Shi, Matthew Squires, Nicoletta Pirotta, Sarah Beall, Andrea Harzstark, Jürgen E. Gschwend, Chia-Chi Lin, Daniel Castellano, Yen-Chuan Ou, Alain Ravaud, Viktor Grünwald, and Bernard Escudier

Abstract

PDF file - 20KB

Published

2023

12. Supplementary Table 1 from Phase II Results of Dovitinib (TKI258) in Patients with Metastatic Renal Cell Cancer

Author

Eric Angevin, Michael Shi, Matthew Squires, Nicoletta Pirotta, Sarah Beall, Andrea Harzstark, Jürgen E. Gschwend, Chia-Chi Lin, Daniel Castellano, Yen-Chuan Ou, Alain Ravaud, Viktor Grünwald, and Bernard Escudier

Abstract

PDF file - 22KB, Supplemental Table 1 contains the pharmacokinetic results from the study.

Published

2023

13. Data from Phase I Study of Dovitinib (TKI258), an Oral FGFR, VEGFR, and PDGFR Inhibitor, in Advanced or Metastatic Renal Cell Carcinoma

Author

Bernard Escudier, Andrea Kay, Michael Shi, Julie Chang, Paramita Sen, Jean-Charles Soria, Daniel Castellano, Andrea Harzstark, Jürgen E. Gschwend, Chia-Chi Lin, Jose A. Lopez-Martin, and Eric Angevin

Abstract

Purpose: Signaling through the fibroblast growth factor (FGF) pathway may account for tumor resistance to antiangiogenic therapies targeting the VEGF pathway. Here, dovitinib (TKI258), a potent oral inhibitor of FGF receptor, VEGF receptor (VEGFR), and platelet-derived growth factor receptor tyrosine kinases, is studied in a dose escalation trial.Experimental Design: Patients with advanced or metastatic renal cell carcinoma (RCC) with predominant clear cell histology were treated with oral dovitinib 500 or 600 mg/day (5-days-on/2-days-off schedule).Results: Twenty heavily pretreated patients (median 3 prior regimens) were enrolled, with 16, 11, and 12 patients having previously received at least 1: VEGFR inhibitor, mTOR inhibitor, and immunotherapy, respectively. Fifteen and 5 patients were treated in 500- and 600-mg cohorts, respectively. Three patients experienced dose-limiting toxicities: grade 2 bradycardia (500 mg), grade 4 hypertensive crisis (600 mg), and grade 3 asthenia with grade 2 nausea and vomiting (600 mg). The most common adverse events related to dovitinib were nausea (75%), diarrhea (70%), vomiting (70%), and asthenia (50%), the majority of which were mild (grade 1 or 2), with grade 3 events 5% or less (except asthenia, 15%) and only one grade 4 event (hypertensive crisis). Two patients achieved a partial response (500 mg), and 12 patients had stable disease, including 2 patients with long lasting disease stabilizations (>1 year) in the 500-mg cohort.Conclusions: Dovitinib was tolerable and showed antitumor activity at a maximum tolerated dose of 500 mg on a 5-days-on/2-days-off schedule in heavily pretreated RCC patients. Clin Cancer Res; 19(5); 1257–68. ©2012 AACR.

Published

2023

14. Supplementary Table 2 from Phase II Results of Dovitinib (TKI258) in Patients with Metastatic Renal Cell Cancer

Author

Eric Angevin, Michael Shi, Matthew Squires, Nicoletta Pirotta, Sarah Beall, Andrea Harzstark, Jürgen E. Gschwend, Chia-Chi Lin, Daniel Castellano, Yen-Chuan Ou, Alain Ravaud, Viktor Grünwald, and Bernard Escudier

Abstract

PDF file - 25KB, Supplemental Table 2 contains a summary of the newly occurring qualitative ECG abnormalities.

Published

2023

15. Data from ASCEND-7: Efficacy and Safety of Ceritinib Treatment in Patients with ALK-Positive Non–Small Cell Lung Cancer Metastatic to the Brain and/or Leptomeninges

Author

Dong-Wan Kim, Michael Shi, Fabrice Branle, Yuanbo Song, Pilar Cazorla Arratia, Felipe K. Hurtado, Pilar Garrido, Chong-Jen Yu, Mark McKeage, Margarita Majem, Rita Chiari, Sergey Orlov, Chao-Hua Chiu, Patrick Y. Wen, Heather A. Wakelee, Martin J. van den Bent, Erin M. Bertino, Fabrice Barlesi, and Laura Q.M. Chow

Abstract

Purpose:Central nervous system metastases are a prominent cause of morbidity and mortality in patients with ALK-positive (ALK+) non–small cell lung cancer (NSCLC). The phase II ASCEND-7 (NCT02336451) study was specifically designed to assess the efficacy and safety of the ALK inhibitor (ALKi) ceritinib in patients with ALK+ NSCLC metastatic to the brain and/or leptomeninges.Patients and Methods:Patients with active brain metastases were allocated to study arms 1 to 4 based on prior exposure to an ALKi and/or prior brain radiation (arm 1: prior radiotherapy/ALKi-pretreated; arm 2: no radiotherapy/ALKi-pretreated; arm 3: prior radiotherapy/ALKi-naïve; arm 4: no radiotherapy/ALKi-naïve). Arm 5 included patients with leptomeningeal carcinomatosis. Patients received ceritinib 750 mg once daily (fasted condition). Primary endpoint was investigator-assessed whole-body overall response rate (ORR) per RECIST v1.1. Secondary endpoints included disease control rate (DCR) and intracranial/extracranial responses.Results:Per investigator assessment, in arms 1 (n = 42), 2 (n = 40), 3 (n = 12), and 4 (n = 44), respectively: whole-body ORRs [95% confidence interval (CI)] were 35.7% (21.6–52.0), 30.0% (16.6–46.5), 50.0% (21.1–78.9), and 59.1% (43.2–73.7); whole-body DCR (95% CI): 66.7% (50.5–80.4), 82.5% (67.2–92.7), 66.7% (34.9–90.1), and 70.5% (54.8–83.2); intracranial ORRs (95% CI): 39.3% (21.5–59.4), 27.6% (12.7–47.2), 28.6% (3.7–71.0), and 51.5% (33.5–69.2). In arm 5 (n = 18), whole-body ORR was 16.7% (95% CI, 3.6–41.4) and DCR was 66.7% (95% CI, 41.0–86.7). Paired cerebrospinal fluid and plasma sampling revealed that ceritinib penetrated the human blood–brain barrier.Conclusions:Ceritinib showed antitumor activity in patients with ALK+ NSCLC with active brain metastases and/or leptomeningeal disease, and could be considered in the management of intracranial disease.See related commentary by Murciano-Goroff et al., p. 2477

Published

2023

16. 105 Prevalence of claudin18.2 and PD-L1 expression in chinese gastric/gastroesophageal junction adenocarcinoma

Author

Linlin Mao, Wei Yi, Xu-Alan Lin, Ying Gu, Zhenzhong Xia, Chuan Qi, Michael Shi, Steven Yu, and Xueming Qian

Published

2022

17. 771 A phase 1, first in human, open-label, dose escalation and dose expansion study of TST005 in patients with locally advanced or metastatic solid tumors

Author

Lei Chen, Anthony Tolcher, Nashat Gabrail, Minal Barve, Xiaohua WU, Jian Zhang, Michael Shi, Chuan Qi, Steven Yu, Jenny Yao, Jianming Wang, and Christopher Cavanaugh

Published

2022

18. Abstract CT225: Surufatinib plus toripalimab for first-line treatment of advanced non-small cell lung cancer (NSCLC) with PD-L1 positive expression: A multicenter, single-arm phase 2 study

Author

Ying Cheng, Lin Shen, Zhendong Chen, Feng Ye, Xianjun Yu, Xing Zhang, Dongmei Ji, Baorui Liu, Lijie Song, Chunjiao Wu, Ming Lu, Wei Chen, Jingxun Wu, Heli Gao, Desheng Weng, Weina Shen, Rutian Li, Minjie Yang, Jinghong Zhou, Haiyan Shi, Panfeng Tan, Songhua Fan, Michael Shi, and Weiguo Su

Subjects

Cancer Research, Oncology

Abstract

Background: Surufatinib (S, a small-molecule inhibitor of VEGFR 1-3, FGFR1 and CSF-1R) plus toripalimab (T, an anti-PD-1 antibody) showed encouraging antitumor activity in solid tumors (Cao YS, 2022). Programmed death ligand 1 (PD-L1) expression is the established biomarker for 1L immune checkpoint inhibitors therapy in advanced NSCLC. We conducted an open-label, multi-cohort, single-arm phase 2 study to evaluate the safety and efficacy of S+T in patients (pts) with advanced solid tumors. Here, we reported the results of advanced NSCLC with PD-L1 positive expression cohort. Methods: Eligible pts had histologically confirmed advanced NSCLC with no prior systemic chemotherapy, PD-L1 positive (defined as PD-L1 TPS expression ≥1% [sp263]), and without EGFR, ALK or ROS1 genetic alteration if non-sq-NSCLC. Enrolled pts received 21-day cycles of S (250 mg orally QD) plus T (240 mg IV, Q3W) until disease progression or intolerable toxicity or the maximum duration of treatment with toripalimab is 24 months. The primary endpoint was objective response rate (ORR) per RECIST 1.1. Results: From July 2020 to September 2021, 55 pts were screened, of whom 23 pts were enrolled and received the treatment of S+T. Median age was 66 years (range: 49-73), 16 (69.6%) were male and 12 (52.2%) had squamous histology. Pts with PD-L1 TPS ≥50% and Conclusion: Surufatinib and toripalimab combination showed a promising antitumor activity in 1L therapy for advanced PD-L1 positive NSCLC with manageable toxicity. This study might represent a potential treatment option for these pts. Clinical trial information: NCT04169672. Citation Format: Ying Cheng, Lin Shen, Zhendong Chen, Feng Ye, Xianjun Yu, Xing Zhang, Dongmei Ji, Baorui Liu, Lijie Song, Chunjiao Wu, Ming Lu, Wei Chen, Jingxun Wu, Heli Gao, Desheng Weng, Weina Shen, Rutian Li, Minjie Yang, Jinghong Zhou, Haiyan Shi, Panfeng Tan, Songhua Fan, Michael Shi, Weiguo Su. Surufatinib plus toripalimab for first-line treatment of advanced non-small cell lung cancer (NSCLC) with PD-L1 positive expression: A multicenter, single-arm phase 2 study [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2023; Part 2 (Clinical Trials and Late-Breaking Research); 2023 Apr 14-19; Orlando, FL. Philadelphia (PA): AACR; Cancer Res 2023;83(8_Suppl):Abstract nr CT225.

Published

2023

19. Abstract 4020: HMPL-760 is a highly potent and selective reversible BTK inhibitor, targeting BTK and BTKC481S in B-cell malignancies

Author

Linfang Wang, Junqing Liang, Zhihu Gao, Jia Hu, Weigang He, Xianwen Yang, Fangfang Mao, Wei Zhang, Ying Yu, Qihang Zhang, Na Yang, Chun Zhang, Jian Wang, Yu Cai, Xiong Li, Weiguo Qing, Guangxiu Dai, Yongxin Ren, Michael Shi, and Weiguo Su

Subjects

Cancer Research, Oncology

Abstract

Introduction: Bruton’s tyrosine kinase (BTK), a member of the Tec family, plays a crucial role in signaling through B-cell receptor (BCR). BTK inhibition blocks BCR signals and prevents B-cell activation and growth. First-generation BTK inhibitors such as ibrutinib covalently binds to a cysteine residue (C481) of BTK. Their most frequent acquired resistance is the development of a serine mutation in the binding site (C481S). Next generation BTK inhibitors such as LOXO-305 and ARQ 531 are being developed to overcome this resistance to first-generation inhibitors. Methods: HMPL-760 was tested in biochemical assays using recombinant human wild type (WT) and C481S mutant BTKs. Its selectivity was carried out using Eurofins Cerep KinaseProfilerTM panel. Cellular activity of HMPL-760 was evaluated in HEK293 cells stably transfected with BTKWT or BTKC481S, and other tumor cell lines, which are either human diffuse large B cell lymphoma (DLBCL) or mantle cell lymphoma (MCL) cell lines. The in vivo antitumor activity and PKPD correlation of HMPL-760 was studied in HBL-1 xenograft mouse models bearing BTKWT or BTKC481S respectively. Results: In biochemical assays, HMPL-760 strongly inhibits BTK kinase activities towards wild-type BTK (BTKWT) and C481S mutant (BTKC481S), and binds to BTK in a reversible way. HMPL-760 demonstrates high selectivity in a panel containing 413 kinases. In cellular assays, HMPL-760 displays strong anti-proliferative activities in B-cell lymphoma cells (TMD-8, OCI-LY10, REC-1, HBL-1 and HBL-1-BTKC481S) harboring either BTKWT or BTKC481S (GI50: 0.0015-0.046 μM). In human whole blood assay, HMPL-760 inhibits activation of B-cells at nanomolar concentrations measured by inhibition of immunoglobulin-induced CD69 expression in CD19+cells. HMPL-760 shows ≥ 10-fold inhibitory potency than ARQ 531 in both BTKWT and BTKC481S cells, and ~3-fold higher inhibitory potency than that of LOXO-305 in BTKC481S cells. In cellular assay by detecting p-BTK after compound washout, HMPL-760 maintains a longer duration of target inhibition than LOXO-305 in both BTK wild type (HBL-1) and BTK mutant (HBL-1-BTKC481S) cell lines. HMPL-760 displays dose-dependent antitumor efficacy in multiple human B cell lymphoma xenograft models in mice when orally administered at 3~50 mg/kg once daily. Complete tumor regression occurs in most of the tested models at the high dose levels. HMPL-760 shows much stronger antitumor efficacy than LOXO-305 and ARQ 531 at similar dose level, which may be associated with HMPL-760’s higher drug exposures and more sustainable inhibition on BTK phosphorylation in the tumor tissues. Conclusion: HMPL-760 is a reversible, selective, highly potent, BTK inhibitor targeting both BTKWT and BTKC481S. The first-in-human Phase 1 clinical trials of HMPL-760 are under way in patients with r/r B-NHL (NCT05190068, NCT05176691). Citation Format: Linfang Wang, Junqing Liang, Zhihu Gao, Jia Hu, Weigang He, Xianwen Yang, Fangfang Mao, Wei Zhang, Ying Yu, Qihang Zhang, Na Yang, Chun Zhang, Jian Wang, Yu Cai, Xiong Li, Weiguo Qing, Guangxiu Dai, Yongxin Ren, Michael Shi, Weiguo Su. HMPL-760 is a highly potent and selective reversible BTK inhibitor, targeting BTK and BTKC481S in B-cell malignancies. [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2023; Part 1 (Regular and Invited Abstracts); 2023 Apr 14-19; Orlando, FL. Philadelphia (PA): AACR; Cancer Res 2023;83(7_Suppl):Abstract nr 4020.

Published

2023

20. Biomarker Testing Patterns and Treatment Outcomes in Patients With Advanced Non-Small Cell Lung Cancer and MET Exon 14 Skipping Mutations: A Descriptive Analysis From the US

Author

Fatemeh Asad Zadeh Vosta Kolaei, Beilei Cai, Hemanth Kanakamedala, Julia Kim, Vitalii Doban, Shiyu Zhang, and Michael Shi

Subjects

Cancer Research, Oncology

Abstract

BackgroundMET exon 14 skipping mutation (METex14) is observed in ~3% of non-small cell lung cancer (NSCLC) cases and has been shown to be an independent poor prognostic factor associated with shorter overall disease-specific survival. Broad molecular testing can identify this biomarker in patients with advanced NSCLC (aNSCLC) and allow patients to be matched with the appropriate targeted therapy. This study examines biomarker testing patterns and clinical outcomes of chemotherapy and immuno-oncology (IO) monotherapy in aNSCLC patients with METex14.MethodsA descriptive retrospective study was conducted using the Flatiron Health–Foundation Medicine Inc. (FMI) clinico-genomic database. Patients with METex14 aNSCLC treated with systemic therapies were included in the biomarker testing analysis. The duration from specimen collection to reported results was assessed for PD-L1– and METex14-tested patients. Clinical outcomes were assessed in patients treated with chemotherapy or IO monotherapy. First-line (1L) and second-line (2L) real-world progression-free survival (rw-PFS) were estimated using Kaplan-Meier analysis.ResultsOf 91 METex14 patients eligible for the biomarker testing analysis, 77% and 60% received PD-L1 and FMI next-generation sequencing (NGS) testing within 3 months post aNSCLC diagnosis. Of those assessed for both PD-L1 and METex14 (n=9), the median duration between specimen collection and reporting was 1 week shorter for PD-L1 than for FMI NGS. Median 1L rw-PFS was 5.7 months (95% CI, 4.6-7.1) and 2.4 months (95% CI, 1.4-3.2) in patients receiving 1L chemotherapy (n=59) and IO monotherapy (n=18), with 3-month 1L rw-PFS rates of 78% and 33%. Median 2L rw-PFS was 3.5 months (95% CI, 1.9-11.1) and 4.7 months (95% CI, 2.8-12.9) in patients receiving 2L chemotherapy (n=16) and IO monotherapy (n=23), with 3-month 2L rw-PFS rates of 54% and 67%.ConclusionsThe median time from biopsy to test results appears 1 week shorter for PD-L1 than for FMI NGS. Chemotherapy and IO monotherapy were the most common regimens utilized but with limited PFS.

Published

2022

21. Morphological and Molecular Defects in Human Three-Dimensional Retinal Organoid Model of X-Linked Juvenile Retinoschisis

Author

Ping Hsing Tsai, Audrey A. Tran, Wann-Neng Jane, Aliaksandr A. Yarmishyn, Yueh Chien, Shih Hwa Chiou, Chi Hsien Peng, Tien Chun Yang, Kang Chieh Huang, Chia-Ching Chang, Thorsten M. Schlaeger, Shih Jen Chen, Won Jing Wang, Jean Cheng Kuo, Karl J. Wahlin, Phan Nguyen Nhi Nguyen, Jyh Feng Lu, Michael Shi, and Mong Lien Wang

Subjects

0301 basic medicine, Retinal degeneration, Male, RS1, induced pluripotent stem cells, Retinoschisis, retinogenesis, retinoschisin, Biology, medicine.disease_cause, Biochemistry, Article, Retina, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Genetics, Organoid, medicine, Humans, Point Mutation, Induced pluripotent stem cell, Eye Proteins, lcsh:QH301-705.5, Cells, Cultured, Gene Editing, Mutation, lcsh:R5-920, retinal organoid, Cilium, X-linked juvenile retinoschisis, Retinal, Cell Biology, medicine.disease, Phenotype, Cell biology, Organoids, 030104 developmental biology, chemistry, lcsh:Biology (General), retinal degeneration, CRISPR/Cas9 gene editing, RETINOSCHISIN, lcsh:Medicine (General), 030217 neurology & neurosurgery, Developmental Biology

Abstract

Summary X-linked juvenile retinoschisis (XLRS), linked to mutations in the RS1 gene, is a degenerative retinopathy with a retinal splitting phenotype. We generated human induced pluripotent stem cells (hiPSCs) from patients to study XLRS in a 3D retinal organoid in vitro differentiation system. This model recapitulates key features of XLRS including retinal splitting, defective retinoschisin production, outer-segment defects, abnormal paxillin turnover, and impaired ER-Golgi transportation. RS1 mutation also affects the development of photoreceptor sensory cilia and results in altered expression of other retinopathy-associated genes. CRISPR/Cas9 correction of the disease-associated C625T mutation normalizes the splitting phenotype, outer-segment defects, paxillin dynamics, ciliary marker expression, and transcriptome profiles. Likewise, mutating RS1 in control hiPSCs produces the disease-associated phenotypes. Finally, we show that the C625T mutation can be repaired precisely and efficiently using a base-editing approach. Taken together, our data establish 3D organoids as a valid disease model., Highlights • hiPSC-derived retinal organoid model recapitulates key features of XLRS • CRISPR/Cas9 correction normalizes RS1 secretion and retinal development • Transcriptome analysis links XLRS to other hereditary retinopathies, Chiou, Schlaeger, and colleagues use hiPSC-derived retinal organoids to model X-linked juvenile retinoschisis. They show that patient hiPSC-derived retinal organoids replicate key pathologies observed in patients, including retinal splitting and photoreceptor deficit. The observed abnormalities were normalized in organoids derived from isogenic CRISPR/Cas9 gene-corrected hiPSCs. This validated XLRS in vitro model could be used to test and optimize therapeutic approaches.

Published

2019

22. Biomarker Testing Patterns and Treatment Outcomes in Patients With Advanced Non-Small Cell Lung Cancer and

Author

Fatemeh, Asad Zadeh Vosta Kolaei, Beilei, Cai, Hemanth, Kanakamedala, Julia, Kim, Vitalii, Doban, Shiyu, Zhang, and Michael, Shi

Abstract

A descriptive retrospective study was conducted using the Flatiron Health-Foundation Medicine Inc. (FMI) clinico-genomic database. Patients withOf 91The median time from biopsy to test results appears 1 week shorter for PD-L1 than for FMI NGS. Chemotherapy and IO monotherapy were the most common regimens utilized but with limited PFS.

Published

2021

23. Adaptive Finite-Difference Interval Estimation for Noisy Derivative-Free Optimization

Author

Hao-Jun Michael Shi, Yuchen Xie, Melody Qiming Xuan, and Jorge Nocedal

Subjects

Computational Mathematics, Optimization and Control (math.OC), Applied Mathematics, FOS: Mathematics, Mathematics - Optimization and Control

Abstract

A common approach for minimizing a smooth nonlinear function is to employ finite-difference approximations to the gradient. While this can be easily performed when no error is present within the function evaluations, when the function is noisy, the optimal choice requires information about the noise level and higher-order derivatives of the function, which is often unavailable. Given the noise level of the function, we propose a bisection search for finding a finite-difference interval for any finite-difference scheme that balances the truncation error, which arises from the error in the Taylor series approximation, and the measurement error, which results from noise in the function evaluation. Our procedure produces reliable estimates of the finite-difference interval at low cost without explicitly approximating higher-order derivatives. We show its numerical reliability and accuracy on a set of test problems. When combined with L-BFGS, we obtain a robust method for minimizing noisy black-box functions, as illustrated on a subset of unconstrained CUTEst problems with synthetically added noise., Comment: 39 pages, 20 tables, 6 figures

Published

2021

24. Ceritinib Efficacy and Safety in Treatment-Naive Asian Patients With Advanced ALK-Rearranged NSCLC: An ASCEND-4 Subgroup Analysis

Author

Te Chun Hsia, Michael Shi, Meng-Chih Lin, Yi-Long Wu, Paramita Sen, Jun Chen, You Lu, Daniel Shao-Weng Tan, Chong-Jen Yu, Chun-Ming Tsai, Sarayut Lucien Geater, Cheng-Ta Yang, Virote Sriuranpong, and Fabrice Branle

Subjects

Pulmonary and Respiratory Medicine, Oncology, medicine.medical_specialty, Randomization, Nausea, medicine.medical_treatment, Subgroup analysis, Ceritinib, NSCLC, lcsh:RC254-282, chemistry.chemical_compound, Internal medicine, medicine, Chemotherapy, business.industry, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Carboplatin, Pemetrexed, ASCEND-4, chemistry, ALK, Vomiting, Original Article, medicine.symptom, business, medicine.drug

Abstract

Introduction In the phase 3 ASCEND-4 study, ceritinib exhibited improved progression-free survival (PFS) by Blinded Independent Review Committee (BIRC) assessment versus the standard first-line chemotherapy in patients with advanced ALK-rearranged NSCLC. Here, we assessed the efficacy and safety of ceritinib in the subgroup of Asian patients from the ASCEND-4 trial. Methods Treatment-naive patients with stage IIIB or IV ALK-rearranged nonsquamous NSCLC were randomized in a one-to-one ratio to receive either oral ceritinib 750 mg/day (fasted) daily or intravenous chemotherapy ([cisplatin 75 mg/m2 or carboplatin area under the curve 5–6 plus pemetrexed 500 mg/m2] every three wk, followed by pemetrexed maintenance). The primary end point was PFS by BIRC assessment. Results Of 376 randomized patients, 158 (42.0%) were Asian (ceritinib arm: N = 76; chemotherapy arm: N = 82). The median time from randomization to the cutoff date (June 24, 2016) was 18.3 months (range = 13.5–34.2) in the Asian subgroup. The median PFS (by BIRC assessment) was 26.3 months (95% confidence interval [CI]: 8.6–not estimable) and 10.6 months (95% CI: 6.7–15.0), with an estimated 34% risk reduction in PFS (hazard ratio = 0.66, 95% CI: 0.41–1.05) in the ceritinib arm versus chemotherapy arm. The most common adverse events of any grade were diarrhea (85.5%), increased alanine aminotransferase and vomiting (73.7% each), and increased aspartate aminotransferase and nausea (69.7% each) in the ceritinib arm, and nausea (49.3%), vomiting (42.7%), and anemia (40.0%) in the chemotherapy arm. Conclusion Ceritinib was effective and safe in treatment-naive Asian patients with advanced ALK-rearranged NSCLC. The findings were largely consistent with that of the overall study population.

Published

2020

25. A phase I study to evaluate the safety, tolerability, and pharmacokinetics of MSB0254 in Chinese patients with solid tumors

Author

Tianshu Liu, Yulong Zheng, Yi Feng, Yiyi Yu, Wei Li, Cheng Xiao, Jiong Qian, Chenyu Mao, Ning Li, Michael Shi, Chuan Qi, LEI Chen, Steven Yu, Jenny Yao, Lingmin Lu, and Jianming Wang

Subjects

Cancer Research, Oncology

Abstract

3023 Background: MSB0254 is a humanized vascular endothelial growth factor receptor 2 (VEGFR-2) monoclonal antibody. MSB0254 inhibits angiogenesis induced by either VEGF-A or –C. This trial is a phase I study to evaluate MSB0254’s safety, tolerability and PK profiles, as well as early anti-cancer activities in Chinese patients with advanced solid tumors. Methods: In this phase I study (NCT04381325), locally advanced or metastatic solid tumor patients failed previous standard treatments were enrolled. In the dose escalation phase, following 3+3 rules, MSB0254 was given intravenously Q2W (every 2 weeks) at 4mg/kg, 8mg/kg, 12mg/kg, 16mg/kg, and Q3W at 20mg/kg. In the dose expansion phase, patients with selected tumor types will be treated with MSB0254 at 16mg/kg Q2W or 20mg/kg Q3W. Primary objectives were to evaluate the safety and tolerability and to identify maximum tolerable dose (MTD) and/or Recommended Phase 2 Dose (RP2D). Secondary objectives included the assessment of pharmacokinetics, immunogenicity, and preliminary efficacy per RECIST1.1. Results: As of 10th Jan, 2022, a total of 22 Chinese patients have been enrolled into the dose escalation phase and treated with MSB0254 at different dose levels from 4-16mg/kg Q2W or 20mg/kg Q3W. MTD was not reached. One DLT was reported in 12mg/kg Q2W dose cohort. A subject with intra-cholangial carcinoma developed G3 (grade 3) upper gastrointestinal hemorrhage on the C1D13. The adverse event was resolved after symptomatic treatment. The most common treatment-emergent adverse events (TEAEs) (>10%) included: hypertension (27.3%), AST increased (27.3%), γ-GGT increased (22.7%), neutrophil count decreased (18.2%), proteinuria (18.2%), WBC count decreased (13.6%), platelet count decreased (13.6%) and anemia (13.6%). Three subjects (13.6%) experienced G3 TEAEs: 1 upper gastrointestinal hemorrhage, 1 anemia and 1 Hypertriglyceridemia. No G4/5 TEAE was observed. And three subjects (13.6%) experienced 3 SAEs: 1 upper gastrointestinal hemorrhage, 1 G2 intestinal obstruction caused hospitalization and 1 G2 fatigue caused hospitalization. MSB0254 displayed a dose proportional pharmacokinetic profile between 4-16 mg/kg Q2W with calculated T1/2 of 6-9 days. Eighteen subjects had at least one tumor assessment per RECIST 1.1 after MSB0254 treatment. Eleven subjects (61.1%) had best response of stable disease (SD). Four of them had stable disease for more than 6 months, including a neuroendocrine tumor (NET), a gastric cancer, an epithelioid hemangioendothelioma (EHE) and a submaxillary gland carcinoma patient. Conclusions: MSB0254 demonstrated a manageable safety profile and preliminary antitumor activity in patients with advanced solid tumors. 16mk/kg Q2W is recommended as RP2D. 20mg/kg Q3W is still under investigation. The study of MSB0254 on the expansion phase in selected tumor patients is ongoing. Clinical trial information: NCT04381325.

Published

2022

26. A phase I clinical trial to evaluate the safety, tolerability, and pharmacokinetics of TST001 in patients with locally advanced or metastatic solid tumors

Author

Nashat Y. Gabrail, Anthony Tolcher, Olatunji B. Alese, Michael Cecchini, Patel Manish, Haeseong Park, Jordan Berlin, Erika P. Hamilton, Yingjie Huang, Lingmin Lu, Jianming Wang, Michael Shi, and Ming F. Tong

Subjects

Cancer Research, Oncology

Abstract

TPS375 Background: In normal conditions, Claudin (CLDN)18.2 is a tight junction protein with expression strictly confined to differentiated epithelial cells in gastric mucosa. CLDN18.2 has been found to be upregulated, and involved in tumor development and progression in a variety of tumor types such as gastric, pancreatic, and bile duct cancer (BTC). The biological characteristics of CLDN18.2 suggest it is an ideal therapeutic target for cancer drug development. IMAB362 is the first anti-CLDN18.2 monoclonal antibody (mAb) of high potency to have been tested in humans and it revealed clinical efficacy in gastric cancer in a phase II study. TST001, a humanized IgG1 mAb, binds to a distinct epitope of CLDN18.2 with higher affinity and mediates CLDN18.2 expressing cancer cell death through antibody-dependent cellular cytotoxicity (ADCC) in comparison with IMAB362; Furthermore, TST001 is produced using an optimized glycoengineering process to increase affinity to FcR. The enhanced binding to CLDN18.2 on tumor cells and FcR on NK cells results in more efficient engagement of the tumor cells with NK cells and antibody mediated cellular cytotoxicity. In preclinical xenograft studies, TST001 displayed potent anti-tumor activities in the tumor models with medium to high level of CLDN18.2 expression and synergy anti-cancer effect with checkpoint inhibitor. A mAb specific for CLDN18.2 was also developed as an IHC based biomarker for patient enrollment in the clinical trials. Methods: This is an open-label, multi-center, phase I clinical trial to evaluate the safety, maximum tolerated dose (MTD), pharmacokinetics (PK) profile and preliminary anti-cancer effect of TST001 in patients with locally advanced or metastatic solid tumors. (NCT04396821) The study consists of two parts: Part A is a 3+3 dose escalation design with sequential dose cohorts of 1, 3, 6, 10mg/kg in Q2W and Q3W schedules. Based on the emerging safety data, higher doses may be proposed for testing. About 27-54 patients will be enrolled. Dose expansion (Part B) will utilize doses of TST001 based on the emerging data from Part A. In Part B, up to 20 patients with CLDN18.2 overexpression per tumor specific cohort will be enrolled to 3 cohorts: A: TST001 single agent in gastric/gastroesophageal junction (G/GEJ) cancer; B: TST001 + nivolumab in G/GEJ cancer; C: TST001 single agent in pancreatic cancer or BTC. All patients in Part B will be selected by CLDN18.2 expression by central lab testing. The safety, anti-tumor activity, and PK will be further assessed in Part B. Enrolment began in July 2020 in the USA and is ongoing in multiple sites. As of 20 September, 2021, 23 subjects were dosed in Part A and the dose of 10mg/kg is being tested. Another phase I study of TST001 single agent and in combination with chemotherapy in patients with metastatic solid tumor is also ongoing in China (NCT04495296).

Published

2022

27. Optimizing Quantization for Lasso Recovery

Author

Deanna Needell, Shenyinying Tu, Hao-Jun Michael Shi, Mindy Case, Xiaoyi Gu, and Yaniv Plan

Subjects

FOS: Computer and information sciences, Computer science, Computer Science - Information Theory, Information Theory (cs.IT), Applied Mathematics, Quantization (signal processing), ComputingMethodologies_IMAGEPROCESSINGANDCOMPUTERVISION, 020206 networking & telecommunications, Data_CODINGANDINFORMATIONTHEORY, 010103 numerical & computational mathematics, 02 engineering and technology, 01 natural sciences, 94A12, 60D05, 90C25, Quantization (physics), Compressed sensing, Lasso (statistics), Signal Processing, 0202 electrical engineering, electronic engineering, information engineering, 0101 mathematics, Electrical and Electronic Engineering, Algorithm

Abstract

This letter is focused on quantized Compressed Sensing, assuming that Lasso is used for signal estimation. Leveraging recent work, we provide a framework to optimize the quantization function and show that the recovered signal converges to the actual signal at a quadratic rate as a function of the quantization level. We show that when the number of observations is high, this method of quantization gives a significantly better recovery rate than standard Lloyd-Max quantization. We support our theoretical analysis with numerical simulations.

Published

2018

28. Filter Design with Adaptation to Time-Delay Parameters for Genetic Regulatory Networks

Author

Qikun Shen, Hongmei Jiao, Junwu Zhu, Michael Shi, and Peng Shi

Subjects

Lyapunov function, 0209 industrial biotechnology, Computer science, Applied Mathematics, 02 engineering and technology, Protein expression, Adaptive filter, symbols.namesake, Filter design, 020901 industrial engineering & automation, Control theory, Adaptive system, 0202 electrical engineering, electronic engineering, information engineering, Genetics, symbols, 020201 artificial intelligence & image processing, Constant (mathematics), Adaptation (computer science), Biotechnology

Abstract

In existing works, the filters designed for delayed genetic regulatory networks contain time delay. If the time delay is unknown, the filters do not work in practical applications. In order to overcome the shortcoming in such existing works, this paper investigates the filter design problem of genetic regulatory networks with unknown constant time delay, and a novel adaptive filter is introduced, which can estimate online not only unknown network parameters but also the unknown time delay. By the Lyapunove approach, it is shown that the estimating errors asymptotically converge to the origin. Finally, simulation results are presented to illustrate the effectiveness of the proposed new design method.

Published

2018

29. Finite-Time Stability Analysis of Reaction-Diffusion Genetic Regulatory Networks with Time-Varying Delays

Author

Xiaofei Fan, Xian Zhang, Michael Shi, and Ligang Wu

Subjects

0209 industrial biotechnology, Mathematical optimization, Time Factors, Gene regulatory network, Stability (learning theory), 02 engineering and technology, Diffusion, symbols.namesake, 020901 industrial engineering & automation, Exponential stability, Gronwall's inequality, Reaction–diffusion system, 0202 electrical engineering, electronic engineering, information engineering, Genetics, Gene Regulatory Networks, Mathematics, Models, Genetic, Applied Mathematics, Regular polygon, Computational Biology, Dirichlet boundary condition, symbols, 020201 artificial intelligence & image processing, Algorithms, Biotechnology, Numerical stability

Abstract

This paper is concerned with the finite-time stability problem of the delayed genetic regulatory networks (GRNs) with reaction-diffusion terms under Dirichlet boundary conditions. By constructing a Lyapunov-Krasovskii functional including quad-slope integrations, we establish delay-dependent finite-time stability criteria by employing the Wirtinger-type integral inequality, Gronwall inequality, convex technique, and reciprocally convex technique. In addition, the obtained criteria are also reaction-diffusion-dependent. Finally, a numerical example is provided to illustrate the effectiveness of the theoretical results.

Published

2017

30. Updated safety and efficacy of MSB2311 (an anti-programmed death-ligand 1 antibody) in Chinese patients with advanced solid tumors and hematological malignancies from a phase 1 study

Author

Chuan Qi, Zhenzhong Xia, Haijun Zhong, Lin Shen, John Huang, Yufeng Li, Xichun Hu, Jian Zhang, Mengde Wang, Dongmei Ji, Michael Shi, Ling Sun, Jifang Gong, Lei Yang, Qingyuan Zhang, Lingmin Lu, Ying Yuan, and Li Xu

Subjects

Cancer Research, Oncology, biology, business.industry, Tumor penetration, Cancer research, biology.protein, Medicine, Antibody, Antigen binding, Ligand (biochemistry), business, Programmed death

Abstract

e14547 Background: MSB2311 is a novel humanized PD-L1 antibody with a unique pH-dependent antigen binding property that enables intra-tumor recycling and potentiates tumor penetration. Methods: Patients with metastatic solid tumors or selected lymphoma progressed on or after standard treatments were enrolled in this phase I study. In dose escalation part, MSB2311 was given at dose levels of 3, 10, and 20 mg/kg intravenously every 3 weeks. At the dose expansion part, patients with enriched biomarker expression, including EBV+, PD-L1+ (TPS≥50%), MSI-High or TMB-High (≥10muts/Mb), were dosed at 20mg/kg Q3W or 10mg/kg Q2W. Primary objectives are to evaluate the safety and tolerability and to identify MTD and RP2D. Secondary objectives include the assessment of pharmacokinetic parameter, immunogenicity, and preliminary anti-cancer activity per RECIST1.1. Results: As of data cutoff by Aug 31, 2020, 33 Chinese patients had been treated, including 27 heavily pre-treated solid tumor patients and 6 lymphoma patients. No dose limiting toxicity was reported and MTD has not been reached. The most common AEs (>20%) included: anemia, hypothyroidism, aspartate aminotransferase elevated, proteinuria, weight loss. 13 patients (39.4%) experienced grade 3 AEs, and 6 patients (18.2%) experienced SAEs. No treatment related grade 4 or 5 event was reported. Of the 17 efficacy evaluable solid tumor patients with biomarker selection, 6 achieved confirmed partial response with 35% ORR: 2/8 (25%) at 10 mg/kg Q2W and 4/9 (44%) at 20 mg/kg Q3W. Additionally, one patient achieved sustained iPR via iRECIST. 4 out of 7 responding patients (including one iPR) achieved tumor shrinkage of more than 50%, 3 of them got durable response (≥24 weeks).1 out of 6 lymphoma patients achieved PR. Conclusions: MSB2311 demonstrated a manageable safety profile and promising preliminary antitumor activity in patients with advanced solid tumors and selected lymphomas. Clinical trial information: NCT04272944.

Published

2021

31. Compositional Embeddings Using Complementary Partitions for Memory-Efficient Recommendation Systems

Author

Dheevatsa Mudigere, Maxim Naumov, Hao-Jun Michael Shi, and Jiyan Yang

Subjects

FOS: Computer and information sciences, Computer Science - Machine Learning, Theoretical computer science, Computer science, business.industry, Deep learning, Codebook, Machine Learning (stat.ML), Computer Science - Information Retrieval, Machine Learning (cs.LG), Set (abstract data type), Statistics - Machine Learning, Feature (machine learning), Embedding, Feature hashing, Artificial intelligence, Representation (mathematics), business, Categorical variable, Information Retrieval (cs.IR)

Abstract

Modern deep learning-based recommendation systems exploit hundreds to thousands of different categorical features, each with millions of different categories ranging from clicks to posts. To respect the natural diversity within the categorical data, embeddings map each category to a unique dense representation within an embedded space. Since each categorical feature could take on as many as tens of millions of different possible categories, the embedding tables form the primary memory bottleneck during both training and inference. We propose a novel approach for reducing the embedding size in an end-to-end fashion by exploiting complementary partitions of the category set to produce a unique embedding vector for each category without explicit definition. By storing multiple smaller embedding tables based on each complementary partition and combining embeddings from each table, we define a unique embedding for each category at smaller memory cost. This approach may be interpreted as using a specific fixed codebook to ensure uniqueness of each category's representation. Our experimental results demonstrate the effectiveness of our approach over the hashing trick for reducing the size of the embedding tables in terms of model loss and accuracy, while retaining a similar reduction in the number of parameters., Comment: 11 pages, 7 figures, 1 table

Published

2019

32. Influence of Gestational Age at Initiation of Antihypertensive Therapy: Secondary Analysis of CHIPS Trial Data (Control of Hypertension in Pregnancy Study)

Author

Anouk Pels, Ben Willem J. Mol, Joel Singer, Terry Lee, Peter von Dadelszen, Wessel Ganzevoort, Elizabeth Asztalos, Laura A. Magee, Amiram Gafni, Andrée Gruslin, Michael Helewa, Eileen Hutton, Shoo Lee, Alexander Logan, Jennifer Menzies, Jean-Marie Moutquin, Kellie Murphy, Evelyne Rey, Sue Ross, Johanna Sanchez, Jim G. Thornton, Ross Welch, Trinh Hoac, Joanne Kirton, Katherine Trigiani, Ainy Zahid, Michael B. Bracken, Patricia Crowley, Lelia Duley, Richard Ehrenkranz, Kevin Thorpe, Sunny Chan, Michael Shi, Shelley Yu, Raquel de Lourdes Martin, Maria Florencia Bassi, Mirta Clara Caruso, Valeria Lagunas, Fernando Vera, Maria Mohedano de Duhalde, Alicia Beatriz Roque, Patricia Roldan, Esteban Marcos Duhalde, Viviana Dip, Jesus Daniel Aguirre, Elba Mirta Alicia Morales, Griselda Itati Abreo, Teresa De Sagastizabal, Carolina Gomez, Nadia Rizzi, Carlos Arias, Ricardo Antonio Bruno, Kassam Mahomed, Alison Drew, Ann Green, Jane Hoare, Bill Hague, Suzette Coat, Caroline Crowther, Peter Muller, Sophie Trenowden, Barry Walters, Claire Parker, Dorothy Graham, Craig Pennell, Eileen Sung, Angela Makris, Gaksoo Lee, Charlene Thornton, Annemarie Hennessy, Louise Farrell, Nelson Sass, Henri Korkes, Dayana Couto Ferreira, Renato Augusto Moreira de Sa, Monique Schmidt Marques Abreu, Rita Guerios Bornia, Nancy Ribeiro da Silva, Fernanda Freitas Oliveira Cardoso, Caio Coelho Marques, Jorge Hornos, Ricardo Leal Davdt, Letícia Germany Paula, Pedro Luis Zanella, Gabrielle Inglis, Ruth Dillon, Ashley Docherty, Anna Hutfield, Keith Still, Sayrin Lalji, Tamara Van Tent, Chris Hotz, Tracy Messmer, Joel G. Ray, Howard Berger, Leanne De Souza, Andrea Lausman, Tatiana Freire-Lizama, Kate Besel, Paul Gibson, Greta Ellsworth, Leslie Miller, T. Lee-Ann Hawkins, Michelle Hladunewich, Anna Rogowsky, Dini Hui, Virginia Collins, Isabelle Delisle, Cora Fanning, Nestor Demianczuk, Rshmi Khurana, Winnie Sia, Catherine Marnoch, Carmen Young, Cheryl Lux, Sophie Perreault, Valerie Tremblay, Sophie Desindes, Anne-Marie Côté, Veronique Dagenais, Heather Clark, Elaine O’Shea, Ruth Rennicks White, Shital Gandhi, Mary-Jean Martin, Cheryl Brush, Gareth Seaward, Jill Newstead-Angel, Judy Brandt, Jocelyne Martel, Kristine Mytopher, Elise Buschau, Erin Keely, Patti Waddell, Svetlana Shachkina, Alan Karovitch, Robert Anderson, Nicole Koenig, Theresa Yong, Marie Vasiliou, Peri Johnson, Beth Allan, Renato Natale, Laura Kennedy, Lucie Opatrny, Lorraine Lavigne, George Carson, Sheila Kelly, Joan Crane, Donna Hutchens, Juan Pedro Kusanovic, Christian Figueroa, Karla Silva Neculman, Juan Andres Ortiz, Paula Vargas, Pedro Ferrand, Jorge Carrillo, Rodrigo Cifuentes Borrero, Dahiana Marcela Gallo, Luisa Fernanda Moreno, Fred Kirss, Kristiina Rull, Anne Kirss, Tamas Major, Andrea Fodor, Tunde Bartha, Mordechai Hallak, Nardin Aslih, Saja Anabousi-Murra, Ester Pri-Or, Linda Harel, Sima Siev, Marwan Hakim, Christina Simona Khoury, Najla Hamati, Mazen El-Zibdeh, Lama Yousef, Ruth Hughes, Di Leishman, Barbra Pullar, Matthew Farrant, Malgorzata Swiatkowska-Freund, Krzysztof Preis, Anette Aleksandra Traczyk-Los, Anna Partyka, Joanna Preis-Orlikowska, Mariusz Lukaszuk, Grzegorz Krasomski, Michael Krekora, Anna Kedzierska-Markowicz, Katarzyna Zych-Krekora, Grzegorz H. Breborowicz, Anna Dera-Szymanowska, Jannet Bakker, Joost Akkermans, Eline van den Akker, Sabine Logtenberg, Steven Koenen, Maartje de Reus, David Borman, Martijn A. Oudijk, Annemiek Bolte, Viki Verfaille, Bart Graaf, Martina Porath, Corine Verhoeven, Maureen T.M. Franssen, Lida Ulkeman, Ineke Hamming, Jose H.M. Keurentjes, Ina van der Wal, S.W.A. Nij Bijvank, A.A. Lutjes, Henricus Visser, Hubertina Catharina Johanna Scheepers, Erik van Beek, Coby van Dam, Kathy van den Berg-Swart, Paula Pernet, Birgit van der Goes, Nico Schuitemaker, Gunilla Kleiverda, Marcel van Alphen, Ageeth Rosman, Ingrid Gaugler-Senden, Marieke Linders, Catherine Nelson-Piercy, Annette Briley, May Ching Soh, Kate Harding, Hayley Tarft, David Churchill, Katherine Cheshire, Julia Icke, Mausumi Ghosh, James Thornton, Yvonne Toomassi, Karen Barker, Joanne Fisher, Nicky Grace, Amanda Green, Joanne Gower, Anna Molnar, Shobhana Parameshwaran, Andrew Simm, George Bugg, Yvette Davis, Ruta Desphande, Yvette Gunn, Mohammed Houda, Nia Jones, Jason Waugh, Carly Allan, Gareth Waring, Steve A. Walkinshaw, Angela Pascall, Mark Clement-Jones, Michelle Dower, Gillian Houghton, Heather Longworth, Tej Purewal, Derek Tuffnell, Diane Farrar, Jennifer Syson, Gillian Butterfield, Vicky Jones, Rebecca Palethorpe, Tracey Germaine, Marwan Habiba, Debbie Lee, Olufemi Eniola, Lynne Blake, Jane Khan, Helen M. Cameron, Kim Hinshaw, Amanda Bargh, Eileen Walton, Olanrewaju Sorinola, Anna Guy, Zoe D’Souza, Rhiannon Gabriel, Jo Williams, Heidi Hollands, Olujimi Jibodu, Sara Collier, Pauline Tottie, Claire Oxby, James Dwyer, Franz Majoko, Helen Goldring, Sharon Jones, Janet Cresswell, Louise Underwood, Mary Kelly-Baxter, Rebecca Robinson, Dilly Anumba, Anne Chamberlain, Clare Pye, Clare Tower, Sue Woods, Lisa Horrocks, Fiona Prichard, Lynsey Moorhead, Sarah Lee, Louise Stephens, Cara Taylor, Suzanne Thomas, Melissa Whitworth, Jenny Myers, Ellen Knox, Katie Freitas, Mark Kilby, Amanda Cotterill, Khalil Abdo, Katrina Rigby, Julie Butler, Fiona Crosfill, Sean Hughes, Sanjeev Prashar, Fatimah Soydemir, Janet Ashworth, Lorraine Mycock, Jill Smith, Amaju Ikomi, Kerry Goodsell, Jean Byrne, Maxwell Masuku, Alice Pilcher, Meena Khandelwal, Gunda Simpkins, Michelle Iavicoli, Yon Sook Kim, Richard Fischer, Robin Perry, Eugene Y. Chang, Tamara D. Saunders, Betty W. Oswald, Kristin D. Zaks, Sarosh Rana, Dawn McCullough, Anna Sfakianaki, Cheryl Danton, Erin Kustan, Luisa Coraluzzi, Helen How, Christina Waldon, Jeffrey Livingston, Sherry Jackson, Lisa Greene, Dinesh Shah, Jorge E. Tolosa, Monica Rincon, Leonardo Pereira, Amy E. Lawrence, Janice E. Snyder, D. Michael Armstrong, Teresa Blue, Austin Hester, Kathryn Salisbury, Obstetrics and gynaecology, APH - Quality of Care, Amsterdam Reproduction & Development (AR&D), Midwifery Science, Graduate School, Obstetrics and Gynaecology, and APH - Digital Health

Subjects

Gestational hypertension, medicine.medical_specialty, Randomization, Hypertension in Pregnancy, Birth weight, artikel tijdschrift, Preeclampsia, fetal growth restriction, preeclampsia, 03 medical and health sciences, 0302 clinical medicine, Internal Medicine, medicine, hypertension pregnancy-induced, 030212 general & internal medicine, humans, Pregnancy, 030219 obstetrics & reproductive medicine, pregnancy outcome, Obstetrics, business.industry, Gestational age, blood pressure, medicine.disease, 3. Good health, Blood pressure, business

Abstract

For hypertensive women in CHIPS (Control of Hypertension in Pregnancy Study), we assessed whether the maternal benefits of tight control could be achieved, while minimizing any potentially negative effect on fetal growth, by delaying initiation of antihypertensive therapy until later in pregnancy. For the 981 women with nonsevere, chronic or gestational hypertension randomized to less-tight (target diastolic blood pressure, 100 mm Hg), or tight (target, 85 mm Hg) control, we used mixed-effects logistic regression to examine whether the effect of less-tight (versus tight) control on major outcomes was dependent on gestational age at randomization, adjusting for baseline factors as in the primary analysis and including an interaction term between gestational age at randomization and treatment allocation. Gestational age was considered categorically (quartiles) and continuously (linear or quadratic form), and the optimal functional form selected to provide the best fit to the data based on the Akaike information criterion. Randomization before (but not after) 24 weeks to less-tight (versus tight) control was associated with fewer babies with birth weight P interaction =0.005), but more preterm birth ( P interaction =0.043), and no effect on perinatal death or high-level neonatal care >48 hours ( P interaction =0.354). For the mother, less-tight (versus tight) control was associated with more severe hypertension at all gestational ages but particularly so before 28 weeks ( P interaction =0.076). In women with nonsevere, chronic, or gestational hypertension, there seems to be no gestational age at which less-tight (versus tight) control is the preferred management strategy to optimize maternal or perinatal outcomes. Clinical Trial Registration— URL: https://www.isrctn.com . Unique identifier: ISRCTN71416914.

Published

2018

33. First-line ceritinib versus chemotherapy in patients (pts) with advanced ALK rearranged (ALK+) non-small cell lung cancer (NSCLC): ASCEND-4 Asian subgroup analysis

Author

C.-T. Yang, Sarayut Lucien Geater, Paramita Sen, Meng-Chih Lin, Daniel Shao-Weng Tan, You Lu, T. Hsia, Jian Zhou, C. Yu, Michael Shi, Jianxing He, J. Chen, Virote Sriuranpong, Wei Li, Yi-Long Wu, C.-M. Tsai, Fabrice Branle, and P. Yu

Subjects

Chemotherapy, medicine.medical_specialty, Ceritinib, business.industry, medicine.medical_treatment, non-small cell lung cancer (NSCLC), Subgroup analysis, Hematology, medicine.disease, Chemotherapy regimen, Pemetrexed, Oncology, Partial response, Internal medicine, Medicine, business, Progressive disease, medicine.drug

Abstract

Background In global phase III ASCEND-4 study (NCT01283516), ceritinib 750 mg/day (fasted), demonstrated statistically significant and clinically meaningful improvement in PFS by BIRC (median, 16.6 mos [95% CI: 12.6, 27.2] vs 8.1 mos [95% CI: 5.8, 11.1]; HR = 0.55; p Methods Pts with stage IIIB/IV, ALK + (centrally tested IHC), nonsquamous NSCLC, ≥1 measurable lesion per RECIST v1.1, and WHO PS 0–2 were eligible. Efficacy and safety were evaluated in Asian pts who had not received prior systemic anticancer therapy except neo-/adjuvant therapy. Data cutoff: June 24, 2016. Results Among 376 pts randomized (1:1) in the study, 158 pts were Asian, with 76 in ceritinib arm and 82 in chemotherapy arm. Of these, 25 pts (32.9%) in ceritinib arm and 21 (25.6%) in chemotherapy arm had brain metastases at baseline. Median duration of treatment exposure: 64.5 wks (ceritinib, N = 76) and 35.0 wks (chemotherapy, N = 75). Median duration from randomization to data cutoff: 18.3 mos. Ceritinib demonstrated superior PFS by BIRC (median, 26.3 mos; 95% CI: 8.6, NE; HR = 0.66) compared to chemotherapy (Table). Most common (≥50%; all grades; all-causality) AEs in ceritinib arm: diarrhea (85.5%), ALT increased (73.7%), vomiting (73.7%), AST increased (69.7%), and nausea (69.7%). Incidence of grade 3/4 AEs was Table . 1473P By BIRC (N * =158) Ceritinib 750mg N = 76 Chemotherapy N = 82 Overall response rate (ORR), % [95% CI] 65.8 [54.0, 76.3] 29.3 [19.7, 40.4] Best overall response, n (%) Complete response (CR) Partial response (PR) Stable disease (SD) Progressive disease (PD) Non-CR/Non-PD Unknown 0 50 (65.8) 11 (14.5) 11 (14.5) 2 (2.6) 2 (2.6) 0 24 (29.3) 38 (46.3) 6 (7.3) 3 (3.7) 11 (13.4) Disease control rate (DCR), % [95% CI] 82.9 [72.5, 90.6] 79.3 [68.9, 87.4] M ‡ =50 M ‡ =24 Median DOR, months [95% CI] NE [24.7, NE] 16.4 [7.8, NE] n/N (%) 14/50 (28.0) 8/24 (33.3) % Event-free probability estimates [95% CI] 9 months 81.2 [67.0, 89.8] 76.1 [48.0, 90.4] 12 months 79.0 [64.5, 88.1] 50.8 [22.5, 73.5] 15 months 70.4 [54.0, 81.9] 50.8 [22.5, 73.5] Median PFS, months [95% CI] 26.3 [8.6, NE] 10.6 [6.7, 15.0] n/N (%) 32/76 (42.1) 45/82 (54.9) % Event-free probability estimates [95% CI] 9 months 61.0 [48.4, 71.5] 54.7 [41.8, 65.8] 12 months 61.0 [48.4, 71.5] 49.8 [37.1, 61.2] 15 months 55.9 [43.2, 66.9] 39.0 [26.9, 51.0] * Total number of patients included in the full analysis set. ‡ Total number of patients with confirmed complete response or partial response. n: Total number of events included in the analysis. N: Total number of patients included in the analysis. Conclusions In Asian pts with ALK+ NSCLC, ceritinib demonstrated durable and clinically meaningful efficacy and a safety profile consistent with overall ASCEND-4 study results. Clinical trial identification NCT01828099. Editorial acknowledgement Shilpa Garg, Novartis Healthcare Pvt Ltd. Legal entity responsible for the study Novartis Pharmaceuticals Corporation. Funding Novartis Pharmaceuticals Corporation. Disclosure D.S. Tan: Honoraria (self): Merck, Pfizer, Novartis, Boehringer Ingelheim, Roche, Takeda; Advisory / Consultancy: Novartis, Bayer, Boehringer Ingelheim, Celgene, AstraZeneca, Eli-lily, Loxo; Research grant / Funding (self): Novartis, AstraZeneca, GlaxoSmithKline, Bayer, Pfizer; Travel / Accommodation / Expenses: Merck, Pfizer, Novartis, Boehringer Ingelheim, Roche,Takeda. S. Geater: Advisory / Consultancy: Boehringer Ingelheim; Honoraria (institution): AstraZeneca, Boehringer Ingelheim; Research grant / Funding (institution): AstraZeneca, Roche, Novartis, Boehringer Ingelheim; Full / Part-time employment: Prince of Songkla Univerisity. C.J. Yu: Honoraria (self): Roche, AstraZeneca, Ono pharma, Boehringer Ingelheim; Advisory / Consultancy: Roche, AstraZeneca, Ono pharma, Boehringer Ingelheim. T.C. Hsia: Advisory / Consultancy: Norvatis, Lilly, AZ, Roche local speaker. M.C. Lin: Advisory / Consultancy: AZ, Novartis, BI, Roche. V. Sriuranpong: Advisory / Consultancy, Speaker Bureau / Expert testimony: AstraZeneca, Novartis, Roche, Pfizer, Eisai, Boehringer, Taiho, MSD, BMS, Amgen; Research grant / Funding (institution): AstraZeneca, Novartis, Roche, Pfizer, Boehringer, Eisai, Taiho, Lilly, MSD. P. Sen: Shareholder / Stockholder / Stock options, Full / Part-time employment: Novartis. F. Branle: Shareholder / Stockholder / Stock options, Full / Part-time employment: Novartis. M. Shi: Shareholder / Stockholder / Stock options: Novartis stock; Full / Part-time employment: Novartis. Y.L. Wu: Honoraria (self): AZ, Roche, Eli Lilly, Pfizer, MSD, BMS, BI; Advisory / Consultancy: AZ, Roche, BI; Research grant / Funding (institution): AZ, Roche. All other authors have declared no conflicts of interest.

Published

2019

34. Results of the ASCEND-7 phase II study evaluating ALK inhibitor (ALKi) ceritinib in patients (pts) with ALK+ non-small cell lung cancer (NSCLC) metastatic to the brain

Author

Chao-Hua Chiu, C. Yu, Yuanbo Song, M. J. van den Bent, Michael Shi, Dong Wook Kim, Patrick Y. Wen, P. Cazorla Arratia, Fabrice Branle, Laura Q.M. Chow, Erin M. Bertino, Mark J. McKeage, Heather A. Wakelee, Rita Chiari, F.K. Hurtado, Fabrice Barlesi, Sergey Orlov, and Margarita Majem

Subjects

Crizotinib, Ceritinib, medicine.drug_class, business.industry, non-small cell lung cancer (NSCLC), Hematology, medicine.disease, Chemotherapy regimen, ALK inhibitor, Oncology, Response Evaluation Criteria in Solid Tumors, medicine, Cancer research, Progression-free survival, Lung cancer, business, medicine.drug

Published

2019

35. Addressing Health Disparities in Chronic Kidney Disease

Author

I.-Chun Fan, Po-Huang Chiang, Michael Shi-yung Liu, Ta-Chien Chan, and Ming-Daw Su

Subjects

Gerontology, Adult, Male, medicine.medical_specialty, spatial analysis, Adolescent, Health, Toxicology and Mutagenesis, medicine.medical_treatment, prevalence, Taiwan, lcsh:Medicine, urologic and male genital diseases, Article, End stage renal disease, Young Adult, Risk Factors, Environmental health, medicine, Cluster Analysis, Humans, Disease management (health), Renal Insufficiency, Chronic, Dialysis, Aged, geographic information systems, National Insurance, Geography, business.industry, Incidence (epidemiology), Public health, Incidence, lcsh:R, Public Health, Environmental and Occupational Health, Health Status Disparities, Middle Aged, medicine.disease, Health equity, female genital diseases and pregnancy complications, Kidney Failure, Chronic, Female, business, health disparity, chronic kidney disease, Kidney disease

Abstract

According to the official health statistics, Taiwan has the highest prevalence of end stage renal disease (ESRD) in the world. Each year, around 60,000 ESRD patients in Taiwan consume 6% of the national insurance budget for dialysis treatment. The prevalence of chronic kidney disease (CKD) has been climbing during 2008–2012. However, the spatial disparities and clustering of CKD at the public health level have rarely been discussed. The aims of this study are to explore the possible population level risk factors and identify any clusters of CKD, using the national health insurance database. The results show that the ESRD prevalence in females is higher than that in males. ESRD medical expenditure constitutes 87% of total CKD medical expenditure. Pre-CKD and pre-ESRD disease management might slow the progression from CKD to ESRD. After applying ordinary least-squares regression, the percentages of high education status and the elderly in the townships are positively correlated with CKD prevalence. Geographically weighted regression and Local Moran’s I are used for identifying the clusters in southern Taiwan. The findings can be important evidence for earlier and targeted community interventions and reducing the health disparities of CKD.

Published

2014

36. Phase 2 trial of dovitinib in patients with progressive FGFR3-mutated or FGFR3 wild-type advanced urothelial carcinoma

Author

David I. Quinn, Michael Shi, Matthew I. Milowsky, Ignacio Duran, Christian Dittrich, Matthew Squires, Paramita Sen, Linda Cerbone, Satinder Jagdev, Christopher Sweeney, Frederick Millard, Jonathan E. Rosenberg, Dean F. Bajorin, Melissa Lochheed, Cora N. Sternberg, and Walter M. Stadler

Subjects

Male, Urologic Neoplasms, congenital, hereditary, and neonatal diseases and abnormalities, Cancer Research, medicine.medical_specialty, Administration, Oral, Antineoplastic Agents, Quinolones, Gastroenterology, Drug Administration Schedule, Internal medicine, medicine, Humans, Receptor, Fibroblast Growth Factor, Type 3, Neoplasm Metastasis, Stage (cooking), Adverse effect, Aged, business.industry, Wild type, Combination chemotherapy, Middle Aged, Fibroblast growth factor receptor 3, Confidence interval, Surgery, Treatment Outcome, Oncology, Pharmacodynamics, Mutation, Benzimidazoles, Female, business, Tyrosine kinase

Abstract

Background Second-line treatment options for patients with advanced urothelial carcinoma (UC) are limited. Fibroblast growth factor receptor 3 (FGFR3) is dysregulated in UC by activating mutations or protein overexpression in non-mutant tumours. In this study, the efficacy, pharmacodynamics and safety of dovitinib—a broad-targeted inhibitor of tyrosine kinases, including FGFR3—were evaluated in patients with previously treated advanced UC with and without FGFR3 mutations. Methods Forty-four adults with advanced UC who had progressed after one to three platinum-based and/or combination chemotherapy regimens were classified as having mutant ( FGFR3 MUT ; n =12), wild-type ( FGFR3 WT ; n =31), or unknown ( n =1) FGFR3 status. Patients received 500mg dovitinib once daily on a 5-days-on/2-days-off schedule. The primary end-point of this two-stage study was the investigator-assessed overall response rate (ORR). Results Most of the patients were men (75%) and over half of the patients were aged ⩾65years (61%). All patients had received ⩾1 prior antineoplastic therapy for UC. The study was terminated at the end of stage 1, when it was determined by investigator review that the ORR of both the FGFR3 MUT (0%; 95% confidence interval [CI], 0.0–26.5) and FGFR3 WT (3.2%; 95% CI, 0.1–16.7) groups did not meet the criteria to continue to stage 2. The most common grade 3/4 adverse events, suspected to be study-drug related, included thrombocytopenia (9%), fatigue (9%), and asthenia (9%). Conclusion Although generally well tolerated, dovitinib has very limited single-agent activity in patients with previously treated advanced UC, regardless of FGFR3 mutation status. clinicaltrials.gov NCT00790426.

Published

2014

37. Increased Prevalence of Cardiac Allograft Donors with Improved LV Systolic Function Utilizing an Out-of-Hospital Treatment and Recovery Center

Author

Justin Hartupee, Akinobu Itoh, Michael Shi, Joyce Ji, Joel D. Schilling, Shane J. LaRue, Gregory A. Ewald, and Justin M. Vader

Subjects

Organ procurement organization, Out of hospital, Creatinine, medicine.medical_specialty, Ejection fraction, biology, Cardiac allograft, business.industry, Systolic function, Troponin, chemistry.chemical_compound, chemistry, Internal medicine, biology.protein, Cardiology, Medicine, Cardiology and Cardiovascular Medicine, business, Cause of death

Abstract

Background Published data from UNOS demonstrated that donor hearts with transient LV dysfunction can be used without increasing the risk of poor transplant outcomes, but account for less than 3% of allocated donors. Our organ procurement organization (OPO) utilizes a centralized treatment and recovery facility allowing for aggressive protocol driven management and frequent assessment of organ function early after brain death declaration. Methods We retrospectively reviewed our OPO experience with cardiac allograft donors from 2013-2017. Clinical data (patient demographics, cause of death, medical management, biomarkers, and serial echocardiographic imaging) were extracted from the OPO EMR for all 168 allocated cardiac donors during this time period. Improved LV systolic function was defined as an initial LVEF ≤40% which later improved to ≥50% consistent with the definition used in the prior UNOS analysis. Results We found that 23% (38/168) of allocated cardiac allografts from our OPO had transient LV dysfunction with an EF ≤40% on the initial echocardiogram. This rate was consistent over the years examined. Moreover 55% of donors had an initial echocardiogram with an EF of less than 50%. Comparison of donors with an initial EF ≤40% to donors with normal LV function on initial examination revealed minimal differences. There was no difference in the average age or sex between the two groups. No differences were found in the dose of vasopressors used either at the time of arrival to the facility or at organ harvest. The average amount of blood transfused was not different between the two groups. Although peak ALT was significantly higher in donors with transient LV dysfunction (402 vs 175 Units/L), there was no differences found in peak AST, troponin, lactate, or creatinine. Conclusion We found a markedly higher percentage of cardiac donors with transient LV dysfunction in allografts coming from our OPO facility compared to the UNOS database. The extent to which this reflects increased recognition versus increased organ yield is unknown at this time. These donors did not differ significantly from donors with normal LV function on initial examination. Coupled with prior data that showed equivalent outcomes in donors with recovered LV function, these data suggest that additional efforts to recover cardiac allografts initially found to have LV dysfunction could be an important means of increasing the donor pool and further work is ongoing to understand the most important factors in the recovery process.

Published

2018

38. Assessment of drug-drug interaction potential between ceritinib and proton pump inhibitors in healthy subjects and in patients with ALK-positive non-small cell lung cancer

Author

Kalyanee Viraswami-Appanna, Jeffrey W. Scott, Wen Gu, Yvonne Y. Lau, Tiffany Lin, Michael Shi, and Can Cai

Subjects

Adult, Male, Cancer Research, Lung Neoplasms, Adolescent, Subgroup analysis, Antineoplastic Agents, Pharmacology, Toxicology, 030226 pharmacology & pharmacy, Esomeprazole, 03 medical and health sciences, Young Adult, 0302 clinical medicine, Pharmacokinetics, Carcinoma, Non-Small-Cell Lung, Medicine, Anaplastic lymphoma kinase, Humans, Pharmacology (medical), Anaplastic Lymphoma Kinase, Drug Interactions, Dosing, Sulfones, Lung cancer, Protein Kinase Inhibitors, Ceritinib, business.industry, Receptor Protein-Tyrosine Kinases, Proton Pump Inhibitors, Middle Aged, medicine.disease, Healthy Volunteers, Pyrimidines, Treatment Outcome, Oncology, 030220 oncology & carcinogenesis, Concomitant, Area Under Curve, Female, business, medicine.drug

Abstract

The impact of proton pump inhibitors (PPIs) on the pharmacokinetics (PK) and efficacy of ceritinib was evaluated. A healthy subject drug–drug interaction (DDI) study was conducted to assess the effect of esomeprazole on the PK of a single 750 mg dose of ceritinib. To further investigate the impact of PPIs on the PK and efficacy of ceritinib in ALK-positive cancer patients, two subgroup analyses were performed. Analysis 1 evaluated ceritinib steady-state trough concentration (Ctrough,ss) and overall response rate (ORR) by concomitant use of PPIs in patients from the ASCEND-1, -2, and -3 studies; analysis 2 evaluated ceritinib single-dose and steady-state AUC0–24h and C max by concomitant PPI use in patients from ASCEND-1 using a definition of PPI usage similar to that used in the healthy subject study. In the healthy subject study, co-administration of a single 750 mg dose of ceritinib with esomeprazole 40 mg for 6 days decreased ceritinib AUC0–∞ by 76% and C max by 79%. However, based on subgroup analysis 1, patients had similar C trough,ss and ORR regardless of concomitant PPI usage. Based on analysis 2, co-administration of a single 750 mg ceritinib dose with PPIs for 6 days in patients suggested less effect on ceritinib exposure than that observed in healthy subjects as AUC0–24h decreased by 30% and C max decreased by 25%. No clinically meaningful effect on steady-state exposure was observed after daily dosing. Long-term administration of ceritinib with PPIs does not adversely affect the PK and efficacy of ceritinib in ALK-positive cancer patients.

Published

2017

39. Phase I Study of Dovitinib (TKI258), an Oral FGFR, VEGFR, and PDGFR Inhibitor, in Advanced or Metastatic Renal Cell Carcinoma

Author

Eric Angevin, Andrea Kay, Jürgen E. Gschwend, Paramita Sen, Andrea L. Harzstark, Jean-Charles Soria, Chia-Chi Lin, Bernard Escudier, Julie Chang, Michael Shi, Jose A. Lopez-Martin, and Daniel Castellano

Subjects

Adult, Male, Niacinamide, Sorafenib, Cancer Research, medicine.medical_specialty, Maximum Tolerated Dose, Nausea, Drug Evaluation, Preclinical, Mice, Nude, Adenocarcinoma, Quinolones, Gastroenterology, Receptor, Platelet-Derived Growth Factor beta, Mice, Renal cell carcinoma, Internal medicine, Antineoplastic Combined Chemotherapy Protocols, medicine, Carcinoma, Animals, Humans, Tissue Distribution, Receptor, Fibroblast Growth Factor, Type 1, Adverse effect, Carcinoma, Renal Cell, Protein Kinase Inhibitors, Survival rate, Aged, Neoplasm Staging, Vascular Endothelial Growth Factor Receptor-1, business.industry, Phenylurea Compounds, Cancer, Middle Aged, Prognosis, medicine.disease, Kidney Neoplasms, Survival Rate, Endocrinology, Oncology, Vomiting, Benzimidazoles, Female, medicine.symptom, business, Follow-Up Studies, medicine.drug

Abstract

Purpose: Signaling through the fibroblast growth factor (FGF) pathway may account for tumor resistance to antiangiogenic therapies targeting the VEGF pathway. Here, dovitinib (TKI258), a potent oral inhibitor of FGF receptor, VEGF receptor (VEGFR), and platelet-derived growth factor receptor tyrosine kinases, is studied in a dose escalation trial. Experimental Design: Patients with advanced or metastatic renal cell carcinoma (RCC) with predominant clear cell histology were treated with oral dovitinib 500 or 600 mg/day (5-days-on/2-days-off schedule). Results: Twenty heavily pretreated patients (median 3 prior regimens) were enrolled, with 16, 11, and 12 patients having previously received at least 1: VEGFR inhibitor, mTOR inhibitor, and immunotherapy, respectively. Fifteen and 5 patients were treated in 500- and 600-mg cohorts, respectively. Three patients experienced dose-limiting toxicities: grade 2 bradycardia (500 mg), grade 4 hypertensive crisis (600 mg), and grade 3 asthenia with grade 2 nausea and vomiting (600 mg). The most common adverse events related to dovitinib were nausea (75%), diarrhea (70%), vomiting (70%), and asthenia (50%), the majority of which were mild (grade 1 or 2), with grade 3 events 5% or less (except asthenia, 15%) and only one grade 4 event (hypertensive crisis). Two patients achieved a partial response (500 mg), and 12 patients had stable disease, including 2 patients with long lasting disease stabilizations (>1 year) in the 500-mg cohort. Conclusions: Dovitinib was tolerable and showed antitumor activity at a maximum tolerated dose of 500 mg on a 5-days-on/2-days-off schedule in heavily pretreated RCC patients. Clin Cancer Res; 19(5); 1257–68. ©2012 AACR.

Published

2013

40. Established Prevention of Vaso-Occlusive Crises with Crizanlizumab Is Further Improved in Patients Who Follow the Standard Treatment Regimen: Post-Hoc Analysis of the Phase II Sustain Study

Author

Kenneth I. Ataga, Abdullah Kutlar, Federico Campigotto, Andreas Bruederle, Rodolfo D. Cançado, Darla K. Liles, Julie Kanter, and Michael Shi

Subjects

medicine.medical_specialty, education.field_of_study, Intention-to-treat analysis, Randomization, business.industry, Standard treatment, Immunology, Population, Cell Biology, Hematology, Placebo, Biochemistry, Regimen, Internal medicine, Post-hoc analysis, Medicine, business, education, Adverse effect

Abstract

Background: In the 52-week SUSTAIN study, which compared the P-selectin inhibitor crizanlizumab with placebo in patients with sickle cell disease (SCD), crizanlizumab 5.0 mg/kg significantly reduced the frequency of vaso-occlusive crises (VOCs) leading to healthcare utilization versus placebo (Ataga KI et al. N Engl J Med 2017;376:429-39). The overall incidences of adverse events and serious adverse events were similar among the patients treated with crizanlizumab and placebo. Aims: This post-hoc analysis from SUSTAIN evaluated key VOC-related endpoints in crizanlizumab 5.0 mg/kg and placebo groups in the per protocol (PP) population, as a way to assess the effect in patients who are able to follow the standard treatment regimen; data from the intention-to-treat (ITT) population will also be shown for context. Methods: The SUSTAIN study was a randomized, double-blind, placebo-controlled, Phase II study (NCT01895361) that enrolled patients aged 16-65 years with SCD who had experienced 2-10 VOC events in the previous 12 months. Patients were randomized 1:1:1 to receive crizanlizumab 5.0 mg/kg, 2.5 mg/kg or placebo 14 times intravenously over 52 weeks; here we focus on the 5.0 mg/kg dose of crizanlizumab versus placebo. The number and time of VOCs leading to healthcare utilization (e.g., hospital admission, emergency department visit) from randomization to end of treatment were measured for each individual patient. Analyses were conducted on the ITT population (i.e., all patients randomized) and PP population (i.e., all patients randomized who received at least 12/14 planned doses of treatment, and completed the study without major protocol violations that impacted the efficacy assessments). Results: In the crizanlizumab 5.0 mg/kg and placebo groups, there were 67 and 65 patients in the ITT population, and 40 and 41 patients in the PP population, respectively; the main reasons for exclusion from the PP population were associated with violations of the visit schedule. As shown previously (Ataga KI et al. N Engl J Med 2017;376:429-39), the median annual rate of VOCs was 1.63 in the crizanlizumab 5.0 mg/kg group versus 2.98 in the placebo group (stratified Wilcoxon Rank-Sum test, P=0.01; Table) in the ITT population. The median time to first on-treatment VOC was 4.07 versus 1.38 months (stratified log-rank test, P=0.001), respectively, in the crizanlizumab 5.0 mg/kg and placebo groups. Overall, 24/67 (35.8%) and 11/65 (16.9%) patients in the crizanlizumab 5.0 mg/kg and placebo groups (stratified Cochran-Mantel-Haenszel test, P=0.013), respectively, did not experience any VOCs during treatment. In the PP population, the median annual rate of VOCs was 1.04 with crizanlizumab 5.0 mg/kg versus 2.18 with placebo (P=0.02; Table). The median time to first on-treatment VOC was 6.55 months with crizanlizumab 5.0 mg/kg and 1.58 months in the placebo group (P Conclusions: This post-hoc analysis of SUSTAIN shows that crizanlizumab 5.0 mg/kg provided benefit over placebo: nearly halving the median annual rate of VOCs, doubling the time to first VOC, and doubling the number of patients with no VOCs during treatment in the ITT population. The effect was even more pronounced in the PP population. This suggests that the superior VOC-related treatment outcomes of crizanlizumab 5.0 mg/kg versus placebo are further improved in patients who are able to follow the standard crizanlizumab treatment regimen. Disclosures Kanter: NHLBI: Membership on an entity's Board of Directors or advisory committees, Research Funding; Apopharma: Research Funding; Pfizer: Research Funding; bluebird bio: Membership on an entity's Board of Directors or advisory committees, Research Funding; Global Blood Therapeutics: Research Funding; ASH: Membership on an entity's Board of Directors or advisory committees; AstraZeneca: Membership on an entity's Board of Directors or advisory committees; Sancilio: Research Funding; Novartis: Membership on an entity's Board of Directors or advisory committees, Research Funding. Kutlar:Novartis: Consultancy, Honoraria, Other: Personal fees, Research Funding; Sancilio: Other: DSMB Chair; Bluebird Bio: Other: DSMB Member. Bruederle:Novartis: Employment. Shi:Novartis: Employment, Other: Stock owner of Novartis. Campigotto:Novartis: Employment. Ataga:Pfizer: Research Funding; Global Blood Therapeutics: Honoraria, Membership on an entity's Board of Directors or advisory committees, Research Funding; Novartis Pharmaceuticals: Honoraria; Modus Therapeutics: Honoraria; Bioverativ: Honoraria, Membership on an entity's Board of Directors or advisory committees.

Published

2018

41. Practical Algorithms for Learning Near-Isometric Linear Embeddings

Author

Hao-Jun Michael Shi, Jerry Luo, Qi Yang, Kayla Shapiro, and Kan Zhu

Subjects

Unit sphere, FOS: Computer and information sciences, 010102 general mathematics, Regular polygon, Matrix norm, 020206 networking & telecommunications, Machine Learning (stat.ML), 02 engineering and technology, 01 natural sciences, Restricted isometry property, Matrix decomposition, Machine Learning (cs.LG), Distortion (mathematics), Matrix (mathematics), Computer Science - Learning, 90C90, Statistics - Machine Learning, Optimization and Control (math.OC), 0202 electrical engineering, electronic engineering, information engineering, FOS: Mathematics, 0101 mathematics, Finite set, Algorithm, Mathematics - Optimization and Control, Mathematics

Abstract

We propose two practical non-convex approaches for learning near-isometric, linear embeddings of finite sets of data points. Given a set of training points $\mathcal{X}$, we consider the secant set $S(\mathcal{X})$ that consists of all pairwise difference vectors of $\mathcal{X}$, normalized to lie on the unit sphere. The problem can be formulated as finding a symmetric and positive semi-definite matrix $\boldsymbol{\Psi}$ that preserves the norms of all the vectors in $S(\mathcal{X})$ up to a distortion parameter $\delta$. Motivated by non-negative matrix factorization, we reformulate our problem into a Frobenius norm minimization problem, which is solved by the Alternating Direction Method of Multipliers (ADMM) and develop an algorithm, FroMax. Another method solves for a projection matrix $\boldsymbol{\Psi}$ by minimizing the restricted isometry property (RIP) directly over the set of symmetric, postive semi-definite matrices. Applying ADMM and a Moreau decomposition on a proximal mapping, we develop another algorithm, NILE-Pro, for dimensionality reduction. FroMax is shown to converge faster for smaller $\delta$ while NILE-Pro converges faster for larger $\delta$. Both non-convex approaches are then empirically demonstrated to be more computationally efficient than prior convex approaches for a number of applications in machine learning and signal processing.

Published

2016

42. Methods for Quantized Compressed Sensing

Author

Mindy Case, Deanna Needell, Xiaoyi Gu, Hao-Jun Michael Shi, and Shenyinying Tu

Subjects

FOS: Computer and information sciences, Computer science, Information Theory (cs.IT), Numerical analysis, Computer Science - Information Theory, ComputingMethodologies_IMAGEPROCESSINGANDCOMPUTERVISION, 020206 networking & telecommunications, Numerical Analysis (math.NA), 010103 numerical & computational mathematics, 02 engineering and technology, Data_CODINGANDINFORMATIONTHEORY, Information theory, 01 natural sciences, Matching pursuit, Thresholding, Quantization (physics), 94A12, 60D05, 90C25, Compressed sensing, Outlier, FOS: Mathematics, 0202 electrical engineering, electronic engineering, information engineering, Mathematics - Numerical Analysis, 0101 mathematics, Noise level, Algorithm

Abstract

In this paper, we compare and catalog the performance of various greedy quantized compressed sensing algorithms that reconstruct sparse signals from quantized compressed measurements. We also introduce two new greedy approaches for reconstruction: Quantized Compressed Sampling Matching Pursuit (QCoSaMP) and Adaptive Outlier Pursuit for Quantized Iterative Hard Thresholding (AOP-QIHT). We compare the performance of greedy quantized compressed sensing algorithms for a given bit-depth, sparsity, and noise level.

Published

2015

43. A haplotype map of the human genome

Author

Mark Leppert, Aravinda Chakravarti, Charmaine D.M. Royal, Sarah S. Murray, Renzong Qiu, Panos Deloukas, Renwu Wang, David A. Hinds, Barbara E. Stranger, Xiaoli Tang, Huanming Yang, John W. Belmont, Nigel P. Carter, Huy Nguyen, William Mak, Kazuto Kato, Shiran Pasternak, Chaohua Li, Jeffrey C. Barrett, Lon R. Cardon, Vincent Ferretti, Atsushi Nagashima, Peter E. Chen, Stephen F. Schaffner, Hongbo Fu, Zhu Chen, Siqi Liu, John Burton, Paul Hardenbol, Gudmundur A. Thorisson, Yusuke Nakamura, Mark Griffiths, Imtiaz Yakub, Eiko Suda, Gonçalo R. Abecasis, Carl S. Kashuk, Qingrun Zhang, Yoshimitsu Fukushima, Karen Kennedy, Sarah E. Hunt, Yi Wang, Norio Niikawa, Ichiro Matsuda, Lynn F. Zacharia, Lalitha Krishnan, Zhen Wang, Stéphanie Roumy, C M Clee, David J. Cutler, Albert V. Smith, Lincoln Stein, Simon Myers, Jane Peterson, Jun Zhou, Yozo Ohnishi, Weihua Guan, Matthew Stephens, Xiaoyan Xiong, Julian Maller, Houcan Zhang, Pui-Yan Kwok, Mark S. Guyer, Liuda Ziaugra, Jonathan Witonsky, Matthew C. Jones, Stacey Gabriel, You-Qiang Song, Daochang An, Haifeng Wang, Gilean McVean, Lawrence M. Sung, Zhijian Yao, Yan Shen, Yangfan Liu, George M. Weinstock, Ludmila Pawlikowska, Erica Sodergren, Mark T. Ross, Andrew Boudreau, Toshihiro Tanaka, Thomas D. Willis, Weitao Hu, Kelly A. Frazer, Li Jin, Robert W. Plumb, Paul I.W. de Bakker, Hongbin Zhao, Wei Lin, Sarah Sims, Richard A. Gibbs, Maura Faggart, Michael Feolo, Dennis G. Ballinger, Xun Chu, Lucinda Fulton, Marcos Delgado, Ellen Winchester, Wei Huang, Fuli Yu, Christianne R. Bird, Shaun Purcell, Jessica Roy, Dongmei Cai, Launa M. Galver, Bartha Maria Knoppers, Emmanouil T. Dermitzakis, Gao Yang, Takashi Morizono, Rachel Barry, Kirsten McLay, Daryl J. Thomas, Steve McCarroll, Jonathan Marchini, Daniel J. Richter, Andy Peiffer, Patricia Taillon-Miller, Richard K. Wilson, Stephen Kwok-Wing Tsui, Jian-Bing Fan, Lisa D. Brooks, Laura L. Stuve, Paul L'Archevêque, David M. Evans, Clémentine Sallée, Peter Donnelly, Hong Xue, Hui Zhao, Charles N. Rotimi, Jean E. McEwen, J. Tze Fei Wong, Hao Pan, Alastair Kent, Brendan Blumenstiel, Qing Li, Weiwei Sun, L. Kang, Colin Freeman, John Stewart, Chibuzor Nkwodimmah, Morris W. Foster, Don Powell, Leonardo Bottolo, Raymond D. Miller, Stephen T. Sherry, Francis S. Collins, Donna M. Muzny, Jun Yu, Ike Ajayi, Hua Han, Pardis C. Sabeti, Hongguang Wang, Takahisa Kawaguchi, Tatsuhiko Tsunoda, Guy Bellemare, Zhaohui S. Qin, H. B. Hu, Jane Rogers, Thomas J. Hudson, Mark J. Daly, Andrew P. Morris, Supriya Gupta, Ming Xiao, Patrick Varilly, Nick Patterson, Akihiro Sekine, Chris C. A. Spencer, Jonathan Morrison, Missy Dixon, Paul K.H. Tam, Jian Wang, Matthew Defelice, Susana Eyheramendy, Michael Shi, Yungang He, Ellen Wright Clayton, Richa Saxena, Heather M. Munro, Arthur L. Holden, Yayun Shen, Christine P. Bird, Bruce W. Birren, Itsik Pe'er, David R. Bentley, Lynne V. Nazareth, Pamela Whittaker, Pak C. Sham, Amy L. Camargo, David A. Wheeler, Koji Saeki, Martin Godbout, David Altshuler, Liang Xu, Ying Wang, David Willey, Alexandre Montpetit, Shin Lin, Michael S. Phillips, Changqing Zeng, Clement Adebamowo, John C. Wallenburg, Mark S. Chee, Ben Fry, Erich Stahl, Melissa Parkin, Rhian Gwilliam, Andrei Verner, Patrick J. Nailer, Lap-Chee Tsui, Bo Zhang, Fanny Chagnon, David R. Cox, Jack Spiegel, Jamie Moore, Vivian Ota Wang, Patricia A. Marshall, Takuya Kitamoto, Bruce S. Weir, Darryl Macer, Geraldine M. Clarke, Robert C. Onofrio, Mary M.Y. Waye, Wei Wang, Suzanne M. Leal, James C. Mullikin, Toyin Aniagwu, Daniel C. Koboldt, Mary Goyette, Martin Leboeuf, Isaac F. Adewole, Ruth Jamieson, Arnold Oliphant, Jessica Watkin, and Jean François Olivier

Subjects

Linkage disequilibrium, Biology, DNA, Mitochondrial, Polymorphism, Single Nucleotide, Article, Linkage Disequilibrium, Structural variation, Gene Frequency, Humans, Selection, Genetic, International HapMap Project, Genetic association, Haplotypes - genetics, Recombination, Genetic, Genetics, Chromosomes, Human, Y, Multidisciplinary, Genome, Human, DNA, Mitochondrial - genetics, Haplotype, Tag SNP, Polymorphism, Single Nucleotide - genetics, Haplotypes, Human genome, Haplotype estimation, Chromosomes, Human, Y - genetics

Abstract

Inherited genetic variation has a critical but as yet largely uncharacterized role in human disease. Here we report a public database of common variation in the human genome: more than one million single nucleotide polymorphisms (SNPs) for which accurate and complete genotypes have been obtained in 269 DNA samples from four populations, including ten 500-kilobase regions in which essentially all information about common DNA variation has been extracted. These data document the generality of recombination hotspots, a block-like structure of linkage disequilibrium and low haplotype diversity, leading to substantial correlations of SNPs with many of their neighbours. We show how the HapMap resource can guide the design and analysis of genetic association studies, shed light on structural variation and recombination, and identify loci that may have been subject to natural selection during human evolution. © 2005 Nature Publishing Group., link_to_OA_fulltext

Published

2005

44. PREDICTION OF LVAD PUMP THROMBOSIS WITH 30-DAY LDH VALUES: RESULTS FROM A LARGE-VOLUME HIGH ACUITY TRANSPLANT CENTER

Author

Jonathan D. Moreno, Shane J. LaRue, and Michael Shi

Subjects

medicine.medical_specialty, business.industry, medicine.disease, Thrombosis, chemistry.chemical_compound, chemistry, Internal medicine, Lactate dehydrogenase, medicine, Cardiology, Implant, Cardiology and Cardiovascular Medicine, Pump thrombosis, Complication, business

Abstract

Pump thrombosis (PT) remains a life-threatening complication of LVAD therapy. Lactate dehydrogenase (LDH) levels, used to aid in the diagnosis of PT, may rise prior to overt clinical thrombosis. We investigated the predictive power of 30-day post implant LDH to predict future PT. Between 2006 and

Published

2018

45. RISK OF RECURRENT PUMP THROMBOSIS AFTER HEARTMATE II LVAD IMPLANTATION IN A LARGE, HIGH-ACUITY COHORT

Author

Michael Shi, Jonathan D. Moreno, Michael E. Nassif, Justin M. Vader, Shane J. LaRue, David S. Raymer, and Akinobu Itoh

Subjects

medicine.medical_specialty, Heartmate ii, business.industry, Internal medicine, Cohort, Cardiology, Medicine, Cardiology and Cardiovascular Medicine, Pump thrombosis, business

Published

2018

46. Accuracy of Genotyping for Single Nucleotide Polymorphisms by a Microarray-Based Single Nucleotide Polymorphism Typing Method Involving Hybridization of Short Allele-Specific Oligonucleotides

Author

Ryota Ishida, Hironori Iwasaki, Yoichi Ezura, Michael Shi, Jim Knight, Steve Daniel, Mitsuko Kajita, Mitsuru Emi, and Mina Kodaira

Subjects

Genetics, Genotype, Oligonucleotide, Nucleic Acid Hybridization, Reproducibility of Results, Single-nucleotide polymorphism, General Medicine, Biology, Polymerase Chain Reaction, Polymorphism, Single Nucleotide, SNP genotyping, Multiplex polymerase chain reaction, Humans, Typing, DNA microarray, Molecular Biology, Genotyping, Alleles, Oligonucleotide Array Sequence Analysis, SNP array

Abstract

Advances in technologies for identifying genetic polymorphisms rapidly and accurately will dramatically accelerate the discovery of disease-related genes. Among a variety of newly described methods for rapid typing of single-nucleotide polymorphisms (SNPs), gene detection using DNA microarrays is gradually achieving widespread use. This method involves the use of short (11- to 13-mer) allele-specific oligonucleotides. This method allows simultaneous analysis of many SNPs in DNAs from a large number of individuals, in a single experiment. In this work, we evaluated the accuracy of a new microarray-based short allele-specific oligonucleotide (ASO) hybridization method. There is a 96-well formatted array on a single plate, in which up to 256 spots are included in each well. Fluorescent probes for our experiments were produced by multiplex PCR amplification of ten target SNP-containing regions. We genotyped 192 individuals across a panel of ten single base variations, which included an insertion/deletion polymorphism. For comparison, we genotyped the same individuals for the same SNPs by the method of single-base extension with fluorescence detection. The typing accuracies of the microarray-based PCR-ASO and single-base extension methods were calculated as 99.9% and 99.1%, respectively, on the basis of genotyping results determined by direct sequencing. We conclude that the microarray-based hybridization method using short ASO probes represents a potential breakthrough technology for typing large numbers of SNPs rapidly and efficiently.

Published

2002

47. Geographic disparity in chronic obstructive pulmonary disease (COPD) mortality rates among the Taiwan population

Author

Po-Huang Chiang, Michael Shi-yung Liu, Ming-Daw Su, Hsuan-Wen Wang, and Ta-Chien Chan

Subjects

Male, Gerontology, medicine.medical_specialty, Pulmonology, Chronic Obstructive Pulmonary Disease, Population, Taiwan, lcsh:Medicine, Health Informatics, Disease, Research and Analysis Methods, Pulmonary Disease, Chronic Obstructive, Database and Informatics Methods, Altitude, Risk Factors, Epidemiology, Health care, Medicine and Health Sciences, medicine, Humans, Least-Squares Analysis, education, lcsh:Science, Disease burden, education.field_of_study, COPD, Health Care Policy, Multidisciplinary, business.industry, Mortality rate, lcsh:R, Health Status Disparities, medicine.disease, Health Care, Female, lcsh:Q, Disease Registries, business, Research Article, Demography

Abstract

Chronic obstructive pulmonary disease (COPD) causes a high disease burden among the elderly worldwide. In Taiwan, the long-term temporal trend of COPD mortality is declining, but the geographical disparity of the disease is not yet known. Nationwide COPD age-adjusted mortality at the township level during 1999–2007 is used for elucidating the geographical distribution of the disease. With an ordinary least squares (OLS) model and geographically weighted regression (GWR), the ecologic risk factors such as smoking rate, area deprivation index, tuberculosis exposure, percentage of aborigines, density of health care facilities, air pollution and altitude are all considered in both models to evaluate their effects on mortality. Global and local Moran’s I are used for examining their spatial autocorrelation and identifying clusters. During the study period, the COPD age-adjusted mortality rates in males declined from 26.83 to 19.67 per 100,000 population, and those in females declined from 8.98 to 5.70 per 100,000 population. Overall, males’ COPD mortality rate was around three times higher than females’. In the results of GWR, the median coefficients of smoking rate, the percentage of aborigines, PM10 and the altitude are positively correlated with COPD mortality in males and females. The median value of density of health care facilities is negatively correlated with COPD mortality. The overall adjusted R-squares are about 20% higher in the GWR model than in the OLS model. The local Moran’s I of the GWR’s residuals reflected the consistent high-high cluster in southern Taiwan. The findings indicate that geographical disparities in COPD mortality exist. Future epidemiological investigation is required to understand the specific risk factors within the clustering areas.

Published

2014

48. USCACA hosted symposiums at the 7th CACA meeting and the 15th CSCO meeting in Beijing

Author

Wancai Yang, Li Yan, Michael Shi, and Pascal Qian

Subjects

Clinical Oncology, Delegation, business.industry, media_common.quotation_subject, education, Library science, Chinese society, Cancer Early Detection, humanities, Clinical trial, Oncology, Drug development, Beijing, Medicine, business, China, media_common

Abstract

In September 2012, the US Chinese Anti-Cancer Association (USCACA) hosted two symposiums in Beijing. The USCACA hosted the first joint session at the 7th annual meetings of the Chinese Anti-Cancer Association (CACA), themed on "Collaboration between the US and China in Cancer Research." Six experts from the United States and China presented their latest work on basic and translational cancer research. During this symposium, 5 young Chinese scholars, returnees after their training in the United States, were honored the"AFCR-USCACA Scholarships Award." The USCACA hosted a second symposium during the 15th annual meeting of the Chinese Society of Clinical Oncology (CSCO), focused on the "US-China Collaboration in Cancer Drug Clinical Development." An international delegation of oncology experts presented the innovative clinical trial strategies and discussed the biomarkers for cancer early detection and clinical trials, targeted therapy, and new drug development. The Oncology Drug Clinical Development and Safety Evaluation Committee was also launched to promote an innovative environment and to provide a collaborative platform for anti-cancer drug development in China.

Published

2012

49. Abstract OT1-1-15: A phase II study of dovitinib as salvage therapy in patients with stage IV inflammatory breast cancer HER2-negative with local or distant relapse

Author

James L Reuben, James L. Murray, Kenneth W. Culver, Mariana Chavez-MacGregor, Ricardo H. Alvarez, Naoto T. Ueno, Gary J. Whitman, Joe Ensor, Wendy A. Woodward, Savitri Krishnamurty, Kimberly Koenig, Antony Lucci, Michael Shi, Gildy Babiera, Vicente Valero, and S. Jackson

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Chemotherapy, business.industry, medicine.medical_treatment, Cancer, Phases of clinical research, Salvage therapy, medicine.disease, Inflammatory breast cancer, Surgery, Regimen, Breast cancer, Internal medicine, medicine, Breast carcinoma, business

Abstract

Background: Inflammatory breast cancer (IBC) is an aggressive form of breast cancer that accounts for 3 to 5% of all invasive breast tumors in the United States. IBC possesses an increase of proangiogenic factors including vascular endothelial growth factor (VEGF), basic fibroblast growth factor (bFGF), and platelet derived growth factor (PDGF) as compared with non-IBC. In particular, FGF family receptors play a critical role in tumorigenesis, morphogenesis, and inducers of angiogenesis. Dovitinib (TKI258) is an oral tyrosine kinase inhibitor with in vitro IC50 values of approximately 10 nmol/L against FGFR1-3, VEGFR1-3, and PDGFR. These structurally related receptors are important for the growth and survival of endothelial cells during tumor angiogenesis. Trial Design: This is a single institution, single arm phase II study. Patients receive a single daily oral dose of dovitinib 500 mg for 5 consecutive days, followed by a 2-day rest period (5 days on/2 days off schedule). Eligibility: Patients have histological confirmation of breast carcinoma with a clinical diagnosis of IBC based on presence of inflammatory changes in the involved breast, including diffuse erythema and edema (peau d’orange). Pathological evidence of dermal lymphatic invasion should be noted but is not required for diagnosis. HER2-negative. ECOG PS 0-2. Baseline MUGA or echocardiogram scans with LVEF of > 50%. Normal hematology, liver and kidney function laboratory studies. Patients must have received at least 2 chemotherapy lines for metastatic disease and have relapsed. Research Hypothesis: Dovitinib has antitumor activity in patients with HER2-negative advanced IBC. Specific Aims: Primary objective: to determine the disease control rate (CR, PR, and SD). Secondary objective: to evaluate safety profile. Exploratory biomarkers: circulating tumor cells (CTC), CTC undergoing EMT, and cancer stem cells Statistical Methods: The primary endpoint is the six-month disease control rate (ORR) as defined by RECIST 1.1. A response is anyone who experiences SD, CR or PR in the first 6 months. We will conduct this study with Simon’s two-stage design using the mini-max criterion and the response rate will be estimated accordingly. It is assumed that dovitinib will have a target ORR of 30%. An ORR of 10% or lower is considered a failure based on the typical ORR with a second line regimen for IBC and the new regimen will be rejected under this circumstance. When the probability of accepting a "bad" regimen (i.e. response rate < 10%) is 0.05 and the probability of rejecting a "good" regimen (i.e. response rate > 30%) is also 0.10, Simon’s design to minimize the maximum sample size requires 22 patients in the first stage. If two or less patients respond to the treatment, the trial will be stopped and the regimen will be declared as ineffective. If at least three of the first 22 patients respond to the treatment, 11 additional patients will be entered in the study to reach a total of 33 patients. By the end of the study, the new regimen will be rejected if response rate is less than or equal to 6 out of 33 patients and will be accepted otherwise. Present Accrual and Target Accrual: A total of 22 patients were accrued. Target accrual is 33 patients. Citation Format: Ricardo H Alvarez, Mariana Chavez-MacGregor, Joe Ensor, James L Murray, Kimberly Koenig, Savitri Krishnamurty, Antony Lucci, Gildy V Babiera, Wendy Woodward, Gary J Whitman, Summer A Jackson, Michael Shi, Kenneth Culver, James L Reuben, Naoto T Ueno, Vicente Valero. A phase II study of dovitinib as salvage therapy in patients with stage IV inflammatory breast cancer HER2-negative with local or distant relapse [abstract]. In: Proceedings of the Thirty-Seventh Annual CTRC-AACR San Antonio Breast Cancer Symposium: 2014 Dec 9-13; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2015;75(9 Suppl):Abstract nr OT1-1-15.

Published

2015

50. A rank-based randomized phase II design when the phase III design is based on overall survival (OS)

Author

Yunro Chung, Maria Grazia Porro, Michael Shi, Weichao Bao, Fei Ma, Patricia A. Wood, and William Mietlowski

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Phase iii trials, business.industry, Internal medicine, medicine, Phase (waves), Clinical endpoint, Overall survival, Rank (graph theory), business

Abstract

6597 Background: Gan (2013) reported that approximately 27% of 120 randomized phase III trials with a primary endpoint of OS had statistically significant outcomes. Ratain (2005) suggests that the ...

Published

2014