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1. Clinical Validation of the Proenkephalin (PENK) Methylation Urine Test for Monitoring Recurrence of Non–muscle-invasive Bladder Cancer

Author

Hyunho Han, Tae Jeong Oh, Ji Eun Heo, Jongsoo Lee, Won Sik Jang, Seung Hwan Lee, Won Sik Ham, Jaehee Hwang, Sungwhan An, and Young-Deuk Choi

Subjects
PENK methylation, Bladder cancer, Surveillance, Urine-derived DNA, Molecular biomarker, Diseases of the genitourinary system. Urology, RC870-923, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282
Abstract

Background and objective: To assess the effectiveness of a urine-based proenkephalin (PENK) methylation test using linear target enrichment-quantitative methylation-specific polymerase chain reaction (mePENK test) for detection of non–muscle-invasive bladder cancer (NMIBC) recurrence compared to cytology and the NMP22 test. Methods: We first conducted a retrospective case-control study involving 54 patients with primary BC and 29 healthy individuals. We then prospectively enrolled 186 patients (January to December 2022) undergoing cystoscopy surveillance after transurethral resection of bladder tumor, of whom 59 had recurrent tumors. We analyzed voided urine samples for PENK methylation levels in urinary DNA. Cystoscopy with histology was used as the reference standard for assessing the diagnostic accuracy of the mePENK test in detecting BC recurrence. We calculated the sensitivity and specificity using receiver operating characteristic curve analysis. Survival differences were determined using the Kaplan-Meier method and Cox proportional-hazards model. A p < 0.05 was considered statistically significant. Key findings and limitations: In the case-control study, the PENK test had sensitivity of 83.3% and specificity of 100%. For NMIBC patients undergoing cystoscopy surveillance, the sensitivity was 76.3% (95% confidence interval [CI] 63.4–86.4%) and the specificity was 85% (95% CI 77.6–90.7%), outperforming cytology (sensitivity: 28.8%, 95% CI 17.8–42.1%; p < 0.001; specificity: 97.6%, 95% CI 93.2–99.5%) and the NMP22 test (sensitivity: 54.2%, 95% CI 40.7–67.2%; p = 0.016; specificity 81.9%, 95% CI 74.1–88.2%). In the high-risk group, the mePENK test had sensitivity of 89.7% (95% CI 75.8–97.1%) and a negative predictive value of 96.9%. For the group with low/intermediate risk, the sensitivity was 41.7%. In the group with negative cystoscopy, recurrence-free survival was shorter for patients with positive than for those with negative mePENK results (245 vs 503 d), with a hazard ratio of 9.4 (p < 0.001). The main study limitation is the small sample size. Conclusions and clinical implications: The mePENK test showed good performance for detection of NMIBC recurrence and has potential for use for prognosis and prediction. Patient summary: We found that a test used to analyze urine samples showed good performance in detecting recurrence of NMIBC. This noninvasive mePENK test may help in personalized follow-up care for patients with NMIBC.

Published
2024
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2. Phosphodiesterase-5 Inhibitor Use in Robot Assisted Radical Prostatectomy Patients Is Associated with Reduced Risk of Death: A Propensity Score Matched Analysis of 1,058 Patients

Author

Jongsoo Lee, Hye Rim Kim, Ji Eun Heo, Won Sik Jang, Kwang Suk Lee, Sung Ku Kang, Hyunho Han, and Young Deuk Choi

Subjects
erectile dysfunction, phosphodiesterase 5 inhibitors, prostatectomy, prostatic neoplasms, survival, Medicine, Diseases of the genitourinary system. Urology, RC870-923
Abstract

Purpose: We investigated whether the use of a phosphodiesterase-5 inhibitor (PDE5i) after robot assited radical prostatectomy has a survival benefit over non-use patients because there are controversial results on the association between PDE5i use and survival outcomes for prostate cancer patients in literature. Materials and Methods: We designed a retrospective, matched, large-sample cohort study of 5,545 patients who underwent robot assisted radical prostatectomy (RARP) during 2013–2021 in a single institute. The exclusion criteria was patients who were aged >70 years at surgery, American Society of Anesthesiologists (ASA) physical status classification grade 4 or 5, history of other malignancies, patients who started PDE5i 6 months after survery and patients with follow up period less than 24 months after surgery. Among the 1,843 included patients, 1,298 were PDE5i users, and 545 were PDE5i non-users. We performed propensity score matching (PSM) of PDE5i users (n=529) with non-users (n=529) by adjusting for the variables of age, Gleason grade group, pathological T stage, preoperative ASA physical status grade, and International Index of Erectile Function score. Results: There were no significant difference in patient characteristics according to PSM. Kaplan–Meier curve revealed the difference of overall survival for PDE5i users and non-users (clustered log-rank test p

Published
2023
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3. Genetic Testing for Prostate Cancer, Urothelial Cancer, and Kidney Cancer

Author

Hyunho Han, Minyong Kang, Seok-Soo Byun, and Seok Joong Yun

Subjects
genetic testing, kidney neoplasms, urothelial carcinoma, prostatic neoplasms, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282, Diseases of the genitourinary system. Urology, RC870-923
Abstract

As genetic testing plays an increasingly salient role in the realm of cancer diagnosis, prognostication, and treatment, this review aims to elucidate the current landscape and future directions of genetic testing in genitourinary cancers, with a focus on prostate cancer, urothelial carcinoma, and renal cell carcinoma. With the increasing adoption of next-generation sequencing technology, the utilization and access to genetic testing in real-world settings have become critical for practicing urologists and genitourinary oncologists, especially after the approval of poly(ADP-ribose) polymerase inhibitors for prostate cancer and the utilization of immune checkpoint inhibitors. In this rapidly evolving field, this review underscores the clinical value of interpreting genetic variations and the importance of distinguishing between germline and somatic mutations, for whom testing can be prescribed, and which genes should be tested. While the current modus operandi predominantly relies on exome sequencing, we posit that the future of genetic testing in genitourinary cancers will see an expansion to encompass whole-genome sequencing, accounting for structural and regulatory variations that impact gene expression. In the upcoming era of liquid biopsies, we envisage an increase in noninvasive cancer genetic testing for the purposes of diagnosis, prognosis, treatment response, and progression monitoring, supplementing the gold-standard tissue biopsies that provide histologic information. Ultimately, thoroughly interpreting genetic testing results and the subsequent treatment implications necessitates a multidisciplinary approach. This review strives to offer urologists a comprehensive perspective on genetic testing in these prevalent urological cancers, contributing to improved diagnosis, prognosis, and treatment decision-making.

Published
2023
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4. The diverse influences of relaxin-like peptide family on tumor progression: Potential opportunities and emerging challenges

Author

Jungchan Jung and Hyunho Han

Subjects
Relaxin, Insulin-like peptide, Cancer, TME, ECM, Science (General), Q1-390, Social sciences (General), H1-99
Abstract

Relaxin-like peptide family exhibit differential expression patterns in various types of cancers and play a role in cancer development. This family participates in tumorigenic processes encompassing proliferation, migration, invasion, tumor microenvironment, immune microenvironment, and anti-cancer resistance, ultimately influencing patient prognosis. In this review, we explore the mechanisms underlying the interaction between the RLN-like peptide family and tumors and provide an overview of therapeutic approaches utilizing this interaction.

Published
2024
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5. Noninvasive studies may have potential to replace cystoscopy in non-muscle invasive bladder cancer follow-up

Author

Jongsoo Lee, Ji Eun Heo, Sung Ku Kang, Kwang Suk Lee, Hyunho Han, Won Sik Jang, and Young Deuk Choi

Subjects
Medicine, Science
Abstract

Abstract Bladder cancer has a high recurrence rate which requires frequent follow-up. Cystoscopy is currently the gold standard for follow-up which is invasive and undesirable procedure for patients. We aimed to investigate the feasibility of noninvasive studies for follow-up of non-muscle invasive bladder cancer. This retrospective study was done for non-muscle invasive bladder cancer patients with abnormal lesion at follow up cystoscopy, therefore those needed transurethral resection of bladder tumor (TUR-BT). Inclusion criteria was patients who had preoperative bladder magnetic resonance imaging (MRI) within 1 month to TUR-BT and urine cytology results. MRI, urine cytology, and surgical pathology results were analyzed for sensitivity, specificity, positive and negative predictive values, accuracy, diagnostic odds ratio, and number needed to misdiagnose for the diagnostic performance of non-invasive studies. From total of 2,258 TUR-BT cases, 1,532 cases of primary TUR-BT and 481 cases which bladder MRI were not done was excluded. Finally, 245 cases of TUR-BT were included. Combined urine cytology and bladder MRI showed 96% sensitivity, 43% specificity, 89% positive and 67% negative predictive values, 87% accuracy, 16.2 diagnostic odds ratio, and 7.4 number needed to misdiagnose values. Among nine false-negative cases, three (1.2%) were missed by the radiologist, two (0.8%) had an empty bladder during magnetic resonance imaging, and three (1.2%) had gross hematuria which needed cystoscopy despite of bladder MRI or urine cytology result. Only one case (0.4%) was missed based on symptoms and noninvasive tests. However, none of the false-negative cases showed rapid extensive progression requiring radical or partial cystectomy. The combination of bladder MRI and urine cytology was comparable to cystoscopy for the follow-up of recurred lesions in non-muscle invasive bladder cancer patients for sensitivity, but not for specificity. However, it may reduce the need for cystoscopy and allowing patients to have choices for follow up diagnostic methods. Also, additional imaging tests to evaluate kidney, ureter and peri-vesical lesions can be reduced.

Published
2022
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6. Optical genome mapping identifies clinically relevant genomic rearrangements in prostate cancer biopsy sample

Author

Yeeun Shim, Jongsoo Lee, Jieun Seo, Cheol Keun Park, Saeam Shin, Hyunho Han, Seung-Tae Lee, Jong Rak Choi, Byung Ha Chung, and Young Deuk Choi

Subjects
Prostate cancer, Optical genome mapping, Structural variation, Genomic rearrangement, BRCA2, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282, Cytology, QH573-671
Abstract

Abstract Background Prostate cancer (PCa) is characterized by complex genomic rearrangements such as the ETS oncogene family fusions, yet the clinical relevance is not well established. While paneled genetic tests of DNA repair genes are recommended in advanced PCa, conventional genomic or cytogenetic tools are not ideal for genome-wide screening of structural variations (SVs) such as balanced translocation due to cost and/or resolution issues. Methods In this study, we tested the feasibility of whole-genome optical genomic mapping (OGM), a newly developed platform for genome-wide SV analysis to detect complex genomic rearrangements in consecutive unselected PCa samples from MRI/US-fusion targeted biopsy. Results We tested ten samples, and nine (90%) passed quality check. Average mapping rate and coverage depth were 58.1 ± 23.7% and 157.3 ± 97.7×, respectively (mean ± SD). OGM detected copy number alterations such as chr6q13 loss and chr8q12-24 gain. Two adjacent tumor samples were distinguished by inter/intra-chromosomal translocations, revealing that they’re from the same ancestor. Furthermore, OGM detected large deletion of chr13q13.1 accompanied by inter-chromosomal translocation t(13;20)(q13.1;p13) occurring within BRCA2 gene, suggesting complete loss of function. Conclusion In conclusion, clinically relevant genomic SVs were successfully detected in PCa samples by OGM. We suggest that OGM can complement panel sequencing of DNA repair genes BRCA1/2 or ATM in high-risk PCa.

Published
2022
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7. Prediction of Postoperative Creatinine Levels by Artificial Intelligence after Partial Nephrectomy

Author

Tae Young Shin, Hyunho Han, Hyun-Seok Min, Hyungjoo Cho, Seonggyun Kim, Sung Yul Park, Hyung Joon Kim, Jung Hoon Kim, and Yong Seong Lee

Subjects
artificial intelligence, acute kidney injury, postoperative renal function, partial nephrectomy, Medicine (General), R5-920
Abstract

Background and Objectives: Multiple factors are associated with postoperative functional outcomes, such as acute kidney injury (AKI), following partial nephrectomy (PN). The pre-, peri-, and postoperative factors are heavily intertwined and change dynamically, making it difficult to predict postoperative renal function. Therefore, we aimed to build an artificial intelligence (AI) model that utilizes perioperative factors to predict residual renal function and incidence of AKI following PN. Methods and Materials: This retrospective study included 785 patients (training set 706, test set 79) from six tertiary referral centers who underwent open or robotic PN. Forty-four perioperative features were used as inputs to train the AI prediction model. XG-Boost and genetic algorithms were used for the final model selection and to determine feature importance. The primary outcome measure was immediate postoperative serum creatinine (Cr) level. The secondary outcome was the incidence of AKI (estimated glomerular filtration rate (eGFR) < 60 mL/h). The average difference between the true and predicted serum Cr levels was considered the mean absolute error (MAE) and was used as a model evaluation parameter. Results: An AI model for predicting immediate postoperative serum Cr levels was selected from 2000 candidates by providing the lowest MAE (0.03 mg/dL). The model-predicted immediate postoperative serum Cr levels correlated closely with the measured values (R2 = 0.9669). The sensitivity and specificity of the model for predicting AKI were 85.5% and 99.7% in the training set, and 100.0% and 100.0% in the test set, respectively. The limitations of this study included its retrospective design. Conclusions: Our AI model successfully predicted accurate serum Cr levels and the likelihood of AKI. The accuracy of our model suggests that personalized guidelines to optimize multidisciplinary plans involving pre- and postoperative care need to be developed.

Published
2023
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8. Mesenchymal and stem-like prostate cancer linked to therapy-induced lineage plasticity and metastasis

Author

Hyunho Han, Yan Wang, Josue Curto, Sreeharsha Gurrapu, Sara Laudato, Alekya Rumandla, Goutam Chakraborty, Xiaobo Wang, Hong Chen, Yan Jiang, Dhiraj Kumar, Emily G. Caggiano, Monica Capogiri, Boyu Zhang, Yan Ji, Sankar N. Maity, Min Hu, Shanshan Bai, Ana M. Aparicio, Eleni Efstathiou, Christopher J. Logothetis, Nicholas Navin, Nora M. Navone, Yu Chen, and Filippo G. Giancotti

Subjects
CP: Cancer, Biology (General), QH301-705.5
Abstract

Summary: Bioinformatic analysis of 94 patient-derived xenografts (PDXs), cell lines, and organoids (PCOs) identifies three intrinsic transcriptional subtypes of metastatic castration-resistant prostate cancer: androgen receptor (AR) pathway + prostate cancer (PC) (ARPC), mesenchymal and stem-like PC (MSPC), and neuroendocrine PC (NEPC). A sizable proportion of castration-resistant and metastatic stage PC (M-CRPC) cases are admixtures of ARPC and MSPC. Analysis of clinical datasets and mechanistic studies indicates that MSPC arises from ARPC as a consequence of therapy-induced lineage plasticity. AR blockade with enzalutamide induces (1) transcriptional silencing of TP53 and hence dedifferentiation to a hybrid epithelial and mesenchymal and stem-like state and (2) inhibition of BMP signaling, which promotes resistance to AR inhibition. Enzalutamide-tolerant LNCaP cells re-enter the cell cycle in response to neuregulin and generate metastasis in mice. Combined inhibition of HER2/3 and AR or mTORC1 exhibits efficacy in models of ARPC and MSPC or MSPC, respectively. These results define MSPC, trace its origin to therapy-induced lineage plasticity, and reveal its sensitivity to HER2/3 inhibition.

Published
2022
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9. Generation of a human induced pluripotent stem cell line YCMi004-A from a patient with dilated cardiomyopathy carrying a protein-truncating mutation of the Titin gene and its differentiation towards cardiomyocytes

Author

Sun-Ho Lee, Jaewon Oh, Seung-Tae Lee, Dongju Won, Sangwoo Kim, Hyo-Kyoung Choi, Seok-Jun Kim, Hyunho Han, Minjae Yoon, Jong Rak Choi, Ho-Geun Yoon, Sahng Wook Park, Seok-Min Kang, and Seung-Hyun Lee

Subjects
Biology (General), QH301-705.5
Abstract

Dilated cardiomyopathy (DCM) is a heart muscle disease that causes heart failure and is the leading cause for heart transplantation. It is a heart muscle disease resulted from a variety of genetics, toxic, metabolic, and infectious causes. One of the most prevalent genetic causes of DCM is a protein-truncating variant in the Titin gene (TTNtv). We have generated a human-induced pluripotent stem cell (hiPSC) line from patients who underwent heart transplantation due to DCM carrying a TTNtv mutation (c.70051C > T, p.Arg23351Ter) at the age of 20. The generated hiPSCs showed normal karyotype (46, XY) and expression of pluripotency markers, and were differentiated towards cardiomyocytes successfully.

Published
2022
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10. DLMFCOS: Efficient Dual-Path Lightweight Module for Fully Convolutional Object Detection

Author

Beomyeon Hwang, Sanghun Lee, and Hyunho Han

Subjects
convolutional neural network, dual-path lightweight module, object detection, fully convolutional one-stage object detector, feature pyramid, Technology, Engineering (General). Civil engineering (General), TA1-2040, Biology (General), QH301-705.5, Physics, QC1-999, Chemistry, QD1-999
Abstract

Recent advances in convolutional neural network (CNN)-based object detection have a trade-off between accuracy and computational cost in various industrial tasks and essential consideration. However, the fully convolutional one-stage detector (FCOS) demonstrates low accuracy compared with its computational costs owing to the loss of low-level information. Therefore, we propose a module called a dual-path lightweight module (DLM) that efficiently utilizes low-level information. In addition, we propose a DLMFCOS based on DLM to achieve an optimal trade-off between computational cost and detection accuracy. Our network minimizes feature loss by extracting spatial and channel information in parallel and implementing a bottom-up feature pyramid network that improves low-level information detection. Additionally, the structure of the detection head is improved to minimize the computational cost. The proposed method was trained and evaluated by fine-tuning parameters through experiments and using public datasets PASCAL VOC 07 and MS COCO 2017 datasets. The average precision (AP) metric is used for our quantitative evaluation matrix for detection performance, and our model achieves an average 1.5% accuracy improvement at about 33.85% lower computational cost on each dataset than the conventional method. Finally, the efficiency of the proposed method is verified by comparing the proposed method with the conventional method through an ablation study.

Published
2023
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11. Androgen-Independent Prostate Cancer Is Sensitive to CDC42-PAK7 Kinase Inhibition

Author

Hyunho Han, Cheol Keun Park, Young-Deuk Choi, Nam Hoon Cho, Jongsoo Lee, and Kang Su Cho

Subjects
prostate cancer, androgen deprivation therapy, castration-resistant prostate cancer, staints, RNA-binding proteins, Biology (General), QH301-705.5
Abstract

Prostate cancer is a common form of cancer in men, and androgen-deprivation therapy (ADT) is often used as a first-line treatment. However, some patients develop resistance to ADT, and their disease is called castration-resistant prostate cancer (CRPC). Identifying potential therapeutic targets for this aggressive subtype of prostate cancer is crucial. In this study, we show that statins can selectively inhibit the growth of these CRPC tumors that have lost their androgen receptor (AR) and have overexpressed the RNA-binding protein QKI. We found that the repression of microRNA-200 by QKI overexpression promotes the rise of AR-low mesenchymal-like CRPC cells. Using in silico drug/gene perturbation combined screening, we discovered that QKI-overexpressing cancer cells are selectively vulnerable to CDC42-PAK7 inhibition by statins. We also confirmed that PAK7 overexpression is present in prostate cancer that coexists with hyperlipidemia. Our results demonstrate a previously unseen mechanism of action for statins in these QKI-expressing AR-lost CRPCs. This may explain the clinical benefits of the drug and support the development of a biology-driven drug-repurposing clinical trial. This is an important finding that could help improve treatment options for patients with this aggressive form of prostate cancer.

Published
2022
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13. Relationship between the experience of online game genre and high risk of Internet gaming disorder in Korean adolescents

Author

Hyunho Han, Hyunsuk Jeong, Sun-Jin Jo, Hye Jung Son, and Hyeon Woo Yim

Subjects
adolescent, online game, internet gaming disorder, game genre, Medicine
Abstract

OBJECTIVES This study examined the association between high risk of Internet gaming disorder (IGD) and online game genres used by adolescents. METHODS The data derived from the baseline data of the Internet user Cohort for Unbiased Recognition of gaming disorder in Early Adolescence. A total 1,532 middle school students who use online games included. The participants reported the names of the online games they used during the past year. Game genres were categorized into role playing games (RPGs), shooting, multiplayer online battle arena (MOBA), simulation, arcade, sports and action games. The risk of IGD was measured using the Internet Gaming Use-Elicited symptom Screen. The relationship between the experience of online game genre and high risk of IGD was analyzed using multiple logistic regression model. RESULTS The game time of a student was longer if he or she had an experience of RPGs, shooting games, MOBA games, simulation games, and action games. The direct and independent association between high risk of IGD in adolescents and the genres of RPGs, simulation games and MOBA were found to be odds ratios 1.52 (95% confidence interval [CI], 1.03 to 2.26); 1.59 (95% CI, 1.03 to 2.45); and 1.51 (95% CI, 1.03 to 2.21), respectively after adjusted the potential confounding variables and the use of other online game genres. CONCLUSIONS The present cross-sectional study has found an association between online game genres and the risk of IGD in adolescents attending a school. A cohort study should verify the causal association in future.

Published
2020
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14. p53 Immunohistochemistry and Mutation Types Mismatching in High-Grade Serous Ovarian Cancer

Author

Eunhyang Park, Hyunho Han, Sung-Eun Choi, Hyunjin Park, Ha-Young Woo, Mi Jang, Hyo-Sup Shim, Sohyun Hwang, Haeyoun Kang, and Nam-Hoon Cho

Subjects
p53, immunohistochemistry, next generation sequencing, oligomerization domain, Medicine (General), R5-920
Abstract

High-grade serous carcinoma (HGSCa) of the ovary is featured by TP53 gene mutation. Missense or nonsense mutation types accompany most cases of HGSCa that correlate well with immunohistochemical (IHC) staining results—an all (missense) or none (nonsense) pattern. However, some IHCs produce subclonal or mosaic patterns from which TP53 mutation types, including the wild type of the gene, cannot be clearly deduced. We analyzed a total of 236 cases of ovarian HGSCa and tumors of other histology by matching the results of p53 IHC staining and targeted next-generation sequencing (TruSight Tumor 170 panel). Ambiguous IHCs that do not belong to the conventional “all or none” groups were reviewed to distinguish the true wild type (WT) from potentially pathogenic subclonal or mosaic patterns. There were about 9% of sequencing-IHC mismatching cases, which were enriched by the p53 c-terminal encoding nuclear localization signal and oligomerization domain, in which the subcellular locations of p53 protein were affected. Indeed, mutations in the oligomerization domain of the p53 protein frequently revealed an unmatched signal or cytosolic staining (L289Ffs*57 (Ins), and R342*). We conclude that both mutation types and IHC patterns of p53 are important sources of information to provide a precise diagnosis of HGSCa.

Published
2022
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15. Efficient Shot Detector: Lightweight Network Based on Deep Learning Using Feature Pyramid

Author

Chansoo Park, Sanghun Lee, and Hyunho Han

Subjects
CNN, EfficientNet, feature pyramid, lightweight deep learning, object detection, Technology, Engineering (General). Civil engineering (General), TA1-2040, Biology (General), QH301-705.5, Physics, QC1-999, Chemistry, QD1-999
Abstract

Convolutional-neural-network (CNN)-based methods are continuously used in various industries with the rapid development of deep learning technologies. However, an inference efficiency problem was reported in applications that require real-time performance, such as a mobile device. It is important to design a lightweight network that can be used in general-purpose environments such as mobile environments and GPU environments. In this study, we propose a lightweight network efficient shot detector (ESDet) based on deep training with small parameters. The feature extraction process was performed using depthwise and pointwise convolution to minimize the computational complexity of the proposed network. The subsequent layer was formed in a feature pyramid structure to ensure that the extracted features were robust to multiscale objects. The network was trained by defining a prior box optimized for the data set of each feature scale. We defined an ESDet-baseline with optimal parameters through experiments and expanded it by gradually increasing the input resolution for detection accuracy. ESDet training and evaluation was performed using the PASCAL VOC and MS COCO2017 Dataset. Moreover, the average precision (AP) evaluation index was used for quantitative evaluation of detection performance. Finally, superior detection efficiency was demonstrated through the experiment compared to the conventional detection method.

Published
2021
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16. EAR-Net: Efficient Atrous Residual Network for Semantic Segmentation of Street Scenes Based on Deep Learning

Author

Seokyong Shin, Sanghun Lee, and Hyunho Han

Subjects
atrous spatial pyramid pooling, deep learning, encoder–decoder, residual learning, semantic segmentation, Technology, Engineering (General). Civil engineering (General), TA1-2040, Biology (General), QH301-705.5, Physics, QC1-999, Chemistry, QD1-999
Abstract

Segmentation of street scenes is a key technology in the field of autonomous vehicles. However, conventional segmentation methods achieve low accuracy because of the complexity of street landscapes. Therefore, we propose an efficient atrous residual network (EAR-Net) to improve accuracy while maintaining computation costs. First, we performed feature extraction and restoration, utilizing depthwise separable convolution (DSConv) and interpolation. Compared with conventional methods, DSConv and interpolation significantly reduce computation costs while minimizing performance degradation. Second, we utilized residual learning and atrous spatial pyramid pooling (ASPP) to achieve high accuracy. Residual learning increases the ability to extract context information by preventing the problem of feature and gradient losses. In addition, ASPP extracts additional context information while maintaining the resolution of the feature map. Finally, to alleviate the class imbalance between the image background and objects and to improve learning efficiency, we utilized focal loss. We evaluated EAR-Net on the Cityscapes dataset, which is commonly used for street scene segmentation studies. Experimental results showed that the EAR-Net had better segmentation results and similar computation costs as the conventional methods. We also conducted an ablation study to analyze the contributions of the ASPP and DSConv in the EAR-Net.

Published
2021
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24. Methodological Rigour in Preclinical Urological Studies: a 14-year systematic review to increase research quality and value

Author

Seung Hyun Park, Se Bee Lee, Seoyeon Park, Eunyoung Kim, Damiano Pizzol, Mike Trott, Yvonne Barnett, Ai Koyanagi, Louis Jacob, Pinar Soysal, Nicola Veronese, Simona Ippoliti, Ramy Abou Ghayda, Nannan Thirumavalavan, Adonis Hijaz, David Sheyn, Rachel Pope, Britt Conroy, Amihay Nevo, Irina Jaeger, Gupta Shubham, Petre-Cristian Ilie, Seung Won Lee, Dong Keon Yon, Hyunho Han, Sung Hwi Hong, Jae Il Shin, Lee Ponsky, and Lee Smith

Abstract

Aims: Methodological rigour enhances reproducibility in preclinical studies and translation from preclinical to clinical studies. We aimed to investigate the prevalence and the trends of essential study design elements in preclinical urological studies, as well as key factors which may improve methodological rigour. Methods and Results: PubMed database was searched, and all the resulting articles in preclinical urological articles published over the past 14-years were reviewed. Total 3768 articles met inclusion criteria. Data on study design elements and animal model used were collected. Citation density and journal impact factor was also examined as a surrogate marker of study influence. We performed analysis on prevalence of seven critical study design elements, and temporal patterns over 14 years. Randomization was reported in 50.0%, blinding in 15.0%, sample size estimation in 1.0%, inclusion of both sexes in 5.7%, statistical analysis in 97.1%, housing and husbandry in 47.7%, and inclusion/exclusion criteria in 5.0%. Temporal analysis showed that the implementation of these study design elements has increased, except for inclusion of both sexes and inclusion/exclusion criteria. Reporting study design elements were not associated with increased citation density. Conclusions: The risk of bias is prevalent in 14-year publications describing preclinical urological research, and the quality of methodological rigour is poorly related to the journal impact factor or the citation of the article. Yet guidelines seem helpful in improving the research quality, because five study design elements (randomization, blinding, sample size estimation, statistical analysis, housing and husbandry) proposed by both NIH and ARRIVE guidelines have been either well reported or improved. Systematic review registration: PROSPERO CRD42022233125 One-sentence summary: Research bias still exists in the fields in preclinical urology, but it is gradually improving.

Published
2022
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25. Characteristics of BRCA2 Mutated Prostate Cancer at Presentation

Author

Hyunho Han, Cheol Keun Park, Nam Hoon Cho, Jongsoo Lee, Won Sik Jang, Won Sik Ham, Young Deuk Choi, and Kang Su Cho

Subjects
Male, BRCA2 Protein, prostate cancer, BRCA2, PSA, Organic Chemistry, Genes, BRCA2, Prostatic Neoplasms, General Medicine, Catalysis, Computer Science Applications, Inorganic Chemistry, Mutation, Humans, Physical and Theoretical Chemistry, Molecular Biology, Spectroscopy, Germ-Line Mutation
Abstract

Genetic alterations of DNA repair genes, particularly BRCA2 in patients with prostate cancer, are associated with aggressive behavior of the disease. It has reached consensus that somatic and germline tests are necessary when treating advanced prostate cancer patients. Yet, it is unclear whether the mutations are associated with any presenting clinical features. We assessed the incidences and characteristics of BRCA2 mutated cancers by targeted sequencing in 126 sets of advanced prostate cancer tissue sequencing data. At the time of diagnosis, cT3/4, N1 and M1 stages were 107 (85%), 54 (43%) and 35 (28%) samples, respectively. BRCA2 alterations of clinical significance by AMP/ASCO/CAP criteria were found in 19 of 126 samples (15.1%). The BRCA2 mutated cancer did not differ in the distributions of TNM stage, Gleason grade group or histological subtype compared to BRCA2 wild-type cancers. Yet, they had higher tumor mutation burden, and higher frequency of ATM and BRCA1 mutations (44% vs. 10%, p = 0.002 and 21% vs. 4%, p = 0.018, respectively). Of the metastatic subgroup (M1, n = 34), mean PSA was significantly lower in BRCA2 mutated cancers than wild-type (p = 0.018). In the non-metastatic subgroup (M0, n = 64), PSA was not significantly different (p = 0.425). A similar trend was noted in multiple metastatic prostate cancer public datasets. We conclude that BRCA2 mutated metastatic prostate cancers may present in an advanced stage with relatively low PSA.

Published
2022

26. LNFCOS: Efficient Object Detection through Deep Learning Based on LNblock

Author

Beomyeon Hwang, Sanghun Lee, and Hyunho Han

Subjects
Computer Networks and Communications, Hardware and Architecture, Control and Systems Engineering, Signal Processing, convolution neural networks, object detection, FCOS, attention method, LNblock, lightweight, Electrical and Electronic Engineering
Abstract

In recent deep-learning-based real-time object detection methods, the trade-off between accuracy and computational cost is an important consideration. Therefore, based on the fully convolutional one-stage detector (FCOS), which is a one-stage object detection method, we propose a light next FCOS (LNFCOS) that achieves an optimal trade-off between computational cost and accuracy. In LNFCOS, the loss of low- and high-level information is minimized by combining the features of different scales through the proposed feature fusion module. Moreover, the light next block (LNblock) is proposed for efficient feature extraction. LNblock performs feature extraction with a low computational cost compared with standard convolutions, through sequential operation on a small amount of spatial and channel information. To define the optimal parameters of LNFCOS suggested through experiments and for a fair comparison, experiments and evaluations were conducted on the publicly available benchmark datasets MSCOCO and PASCAL VOC. Additionally, the average precision (AP) was used as an evaluation index for quantitative evaluation. LNFCOS achieved an optimal trade-off between computational cost and accuracy by achieving a detection accuracy of 79.3 AP and 37.2 AP on the MS COCO and PASCAL VOC datasets, respectively, with 36% lower computational cost than the FCOS.

Published
2022
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27. Prostate epithelial genes define therapy-relevant prostate cancer molecular subtype

Author

Hyung Ho Lee, Kwibok Choi, Won Sik Ham, Won Sik Jang, Koon Ho Rha, Y.D. Choi, Nam Hoon Cho, Hyunho Han, Filippo G. Giancotti, Ji Eun Heo, and Young Jun Moon

Subjects
Male, 0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, Stromal cell, Urology, medicine.medical_treatment, Acid Phosphatase, Cell, Antineoplastic Agents, Docetaxel, Adenocarcinoma, urologic and male genital diseases, Article, Transcriptome, 03 medical and health sciences, Prostate cancer, 0302 clinical medicine, Prostate, Internal medicine, Biomarkers, Tumor, medicine, Humans, Cancer genetics, Retrospective Studies, Chemotherapy, Sequence Analysis, RNA, business.industry, Gene Expression Profiling, Prostatic Neoplasms, Epithelial Cells, Genomics, Prostate-Specific Antigen, medicine.disease, Androgen receptor, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Neoplasm Grading, business, medicine.drug
Abstract

Background and objectives Transcriptomic landscape of prostate cancer (PCa) shows multidimensional variability, potentially arising from the cell-of-origin, reflected in serum markers, and most importantly related to drug sensitivities. For example, Aggressive Variant Prostate Cancer (AVPC) presents low PSA per tumor burden, and characterized by de novo resistance to androgen receptor signaling inhibitors (ARIs). Understanding PCa transcriptomic complexity can provide biological insight and therapeutic guidance. However, unsupervised clustering analysis is hindered by potential confounding factors such as stromal contamination and stress-related material degradation. Materials and methods To focus on prostate epithelial cell-relevant heterogeneity, we defined 1,629 genes expressed by prostate epithelial cells by analyzing publicly available bulk and single- cell RNA sequencing data. Consensus clustering and CIBERSORT deconvolution were used for class discovery and proportion estimate analysis. The Cancer Genome Atlas Prostate Adenocarcinoma dataset served as a training set. The resulting clusters were analyzed in association with clinical, pathologic, and genomic characteristics and impact on survival. Serum markers PSA and PAP was analyzed to predict response to docetaxel chemotherapy in metastatic setting. Results We identified two luminal subtypes and two aggressive variant subtypes of PCa: luminal A (Adipogenic/AR-active/PSA-high) (30.0%); luminal S (Secretory/PAP-high) (26.0%); AVPC-I (Immune-infiltrative) (14.7%), AVPC-M (Myc-active) (4.2%), and mixed (25.0%). AVPC-I and AVPC-M subtypes predicted to be resistant to ARI and have low PSA per tumor burden. Luminal A and AVPC-M predicted to be resistant to docetaxel and have high PSA/PAP Ratio. Metastatic PCa patients with high PSA/PAP ratio (>20) had significantly shorter progression-free survival than those with low ratio (≤20) following docetaxel chemotherapy. Conclusion We propose four prostate adenocarcinoma subtypes with distinct transcriptomic, genomic, and pathologic characteristics. PSA/PAP ratio in advanced cancer may aid in determining which patients would benefit from maximized androgen receptor inhibition or early use of antimicrotubule agents.

Published
2021
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30. Optical genome mapping identifies clinically relevant genomic rearrangements in prostate cancer biopsy sample

Author

Yeeun Shim, Jongsoo Lee, Jieun Seo, Cheol Keun Park, Saeam Shin, Hyunho Han, Seung-Tae Lee, Jong Rak Choi, Byung Ha Chung, and Young Deuk Choi

Subjects
Cancer Research, Oncology, Genetics
Abstract

Background Prostate cancer (PCa) is characterized by complex genomic rearrangements such as the ETS oncogene family fusions, yet the clinical relevance is not well established. While paneled genetic tests of DNA repair genes are recommended in advanced PCa, conventional genomic or cytogenetic tools are not ideal for genome-wide screening of structural variations (SVs) such as balanced translocation due to cost and/or resolution issues. Methods In this study, we tested the feasibility of whole-genome optical genomic mapping (OGM), a newly developed platform for genome-wide SV analysis to detect complex genomic rearrangements in consecutive unselected PCa samples from MRI/US-fusion targeted biopsy. Results We tested ten samples, and nine (90%) passed quality check. Average mapping rate and coverage depth were 58.1 ± 23.7% and 157.3 ± 97.7×, respectively (mean ± SD). OGM detected copy number alterations such as chr6q13 loss and chr8q12-24 gain. Two adjacent tumor samples were distinguished by inter/intra-chromosomal translocations, revealing that they’re from the same ancestor. Furthermore, OGM detected large deletion of chr13q13.1 accompanied by inter-chromosomal translocation t(13;20)(q13.1;p13) occurring within BRCA2 gene, suggesting complete loss of function. Conclusion In conclusion, clinically relevant genomic SVs were successfully detected in PCa samples by OGM. We suggest that OGM can complement panel sequencing of DNA repair genes BRCA1/2 or ATM in high-risk PCa.

Published
2021

31. MP60-18 PROSTATE EPITHELIAL GENES DEFINE DOCETAXEL-SENSITIVE PROSTATE CANCER MOLECULAR SUBTYPE

Author

Won Sik Jang, Kwibok Choi, Nam Hoon Cho, Hyunho Han, Won Sik Ham, Koon Ho Rha, Suki Kang, and Young Deuk Choi

Subjects
Prostate adenocarcinoma, business.industry, Urology, Cancer, medicine.disease, Transcriptome, Prostate cancer, medicine.anatomical_structure, Docetaxel, Prostate, Gene expression, medicine, Cancer research, business, Gene, medicine.drug
Abstract

INTRODUCTION AND OBJECTIVE:Analysis of the transcriptomic landscape of prostate adenocarcinoma has shown multidimensional gene expression variabilities. Understanding the complexity of cancer trans...

Published
2021
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32. Transcriptional Inactivation of TP53 and the BMP Pathway Mediates Therapy-induced Dedifferentiation and Metastasis in Prostate Cancer

Author

Nora M. Navone, Mickey C.T. Hu, Yongying Jiang, Huiqin Chen, Dhiraj Kumar, Hyunho Han, Ana Aparicio, Shanshan Bai, Rumandla A, Curto J, Xiaoping Wang, Bingnan Zhang, Christopher J. Logothetis, Caggiano E, Sankar N. Maity, Sara Laudato, Eleni Efstathiou, Goutam Chakraborty, Filippo G. Giancotti, Yuanxin Wang, Nicholas Navin, Yuan Ji, Ye-Guang Chen, and Sreeharsha Gurrapu

Subjects
Mesenchymal stem cell, mTORC1, Biology, medicine.disease, Metastasis, chemistry.chemical_compound, Prostate cancer, chemistry, Cell culture, Neratinib, medicine, Cancer research, Gene silencing, Enzalutamide, medicine.drug
Abstract

Unsupervised clustering and deconvolution analysis identifies three intrinsic subtypes of Metastatic Castration-Resistant Prostate Cancer (M-CRPC): AR pathway-positive Prostate Cancer (ARPC), Neuro Endocrine Prostate Cancer (NEPC), and a novel subtype endowed with hybrid epithelial/mesenchymal (E/M) and luminal progenitor-like traits (Mesenchymal and Stem-like PC, MSPC). Analysis of large patient datasets and in vitro studies support the notion that MSPC originates from ARPC as a consequence of therapy-induced lineage plasticity. Intriguingly, AR blockade instigates two separate and complementary processes: 1) transcriptional silencing of TP53 and hence acquisition of hybrid E/M and stem-like traits; and 2) inhibition of the BMP-SMAD pathway, which promotes resistance to the pro-apoptotic and anti-proliferative effects of AR inhibition. MSPC cell lines and prostate adenocarcinoma cells reprogrammed in vitro to MSPC exhibit a marked dependency on HER2/3 signaling. Moreover, combinations of the panHER inhibitor neratinib with enzalutamide or the mTORC1 inhibitor MLN0128 exhibit efficacy in preclinical models of mixed ARPC/MSPC or MSPC, respectively. Collectively, these results identify a novel subtype of M-CRPC, trace its origin to therapy induced lineage plasticity, and reveal its dependency on HER2/3 signaling.

Published
2021
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33. Transcriptional Inactivation of TP53 and the BMP Pathway Mediates Therapy-induced Dedifferentiation and Metastasis in Prostate Cancer

Author

Hyunho Han, Yan Wang, Josue Curto, Sreeharsha Gurrapu, Sara Laudato, Alekya Rumandla, Goutam Chakraborty, Xiaobo Wang, Hong Chen, Yan Jiang, Dhiraj Kumar, Emily Caggiano, Boyu Zhang, Yan Ji, Sankar N. Maity, Min Hu, Shanshan Bai, Ana Aparicio, Eleni Efstathiou, Christopher J. Logothetis, Nicholas Navin, Nora Navone, Yu Chen, and Filippo G. Giancotti

Abstract

SummaryUnsupervised clustering and deconvolution analysis identifies a novel subtype of M-CRPC endowed with hybrid epithelial/mesenchymal (E/M) and luminal progenitor-like traits (Mesenchymal and Stem-like PC, MSPC). Analysis of patient datasets and mechanistic studies indicate that MSPC arises as a consequence of therapy-induced lineage plasticity. AR blockade instigates two separate and complementary processes: 1) transcriptional silencing of TP53 and hence acquisition of hybrid E/M and stem-like traits; and 2) inhibition of the BMP signaling, which promotes resistance to the pro-apoptotic and anti-proliferative effects of AR inhibition. The drug-tolerant prostate cancer cells generated through reprogramming are rescued by neuregulin and generate metastases in mice. Combined inhibition of HER2/3 and AR or mTORC1 exhibit efficacy in preclinical models of mixed ARPC/MSPC or MSPC, respectively. These results identify a novel subtype of M-CRPC, trace its origin to therapy-induced lineage plasticity, and reveal its dependency on HER2/3 signaling.

Published
2021
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34. In Vivo Feasibility Test of a New Flexible Ureteroscopic Robotic System, easyUretero, for Renal Stone Retrieval in a Porcine Model.

Author

Joonhwan Kim, Hae Do Jung, Young Joon Moon, Hyunho Han, Byungsik Cheon, Jungmin Han, Sung Yong Cho, Joo Yong Lee, and Dong-Soo Kwon

Abstract

Purpose: Using a new robotic endoscopic platform system developed for retrograde intrarenal surgery (RIRS) called easyUretero (ROEN Surgical Inc.), we evaluated the feasibility and safety of renal stone retrieval in a porcine model. Materials and Methods: Six female pigs were used for our in vivo study. First, 0.3-cm-sized phantom stones were inserted into the kidneys of each pig via the ureteral access sheath. Next, renal stone retrieval was attempted using manual RIRS in three pigs and robotic RIRS in three pigs. Three surgeons performed extraction of 10 stones in each session. Results: The mean stone retrieval time by manual RIRS was significantly shorter than that by robotic RIRS (399.9±185.4 sec vs. 1127.6±374.5 sec, p=0.001). In contrast, the questionnaire regarding usability showed high satisfaction in the surgeons' fatigue category for surgeons using robotic RIRS. The radiation exposure dose was also lower in robotic RIRS than in manual RIRS (0.14 µSv vs. 45.5 µSv). Postoperative ureteral injury assessment revealed Grade 0 in manual RIRS cases and Grades 0, 1, and 2 in robotic RIRS cases. Conclusion: The easyUretero system is a new robotic RIRS system that was developed in Korea. The results of the present study suggest that using easyUretero for stone retrieval during RIRS is safe and ergonomic. [ABSTRACT FROM AUTHOR]

Published
2022
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35. 750 Malat1 lncRNA controls metastatic reactivation of dormant breast cancer by immune evasion

Author

Filippo G. Giancotti, Sreeharsha Gurrapu, Hyunho Han, Yan Wang, Hong Chen, Chang-Jiun Wu, Seong-Yeon Bae PhD, and Dhiraj Kumar

Subjects
MALAT1, Melanoma, Biology, medicine.disease, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Primary tumor, lcsh:RC254-282, Metastasis, Immune system, Tumor progression, medicine, Cancer research, Adenocarcinoma, Cytotoxic T cell
Abstract

Background Long non-coding RNAs (lncRNAs) are involved in various biological processes and diseases. Malat1 (metastasis-associated lung adenocarcinoma transcript 1), also known as Neat2, is one of the most abundant and highly conserved nuclear lncRNAs. Several studies have shown that the expression of lncRNA Malat1 is associated with metastasis and serving as a predictive marker for various tumor progression. Metastatic relapse often develops years after primary tumor removal as a result of disseminated tumor cells undergoing a period of latency in the target organ.1–4 However, the correlation of tumor intrinsic lncRNA in regulation of tumor dormancy and immune evasion is largely unknown. Methods Using an in vivo screening platform for the isolation of genetic entities involved in either dormancy or reactivation of breast cancer tumor cells, we have identified Malat1 as a positive mediator of metastatic reactivation. To functionally uncover the role of Malat1 in metastatic reactivation, we have developed a knock out (KO) model by using paired gRNA CRISPR-Cas9 deletion approach in metastatic breast and other cancer types, including lung, colon and melanoma. As proof of concept we also used inducible knockdown system under in vivo models. To delineate the immune micro-environment, we have used 10X genomics single cell RNA-seq, ChIRP-seq, multi-color flowcytometry, RNA-FISH and immunofluorescence. Results Our results reveal that the deletion of Malat1 abrogates the tumorigenic and metastatic potential of these tumors and supports long-term survival without affecting their ploidy, proliferation, and nuclear speckles formation. In contrast, overexpression of Malat1 leads to metastatic reactivation of dormant breast cancer cells. Moreover, the loss of Malat1 in metastatic cells induces dormancy features and inhibits cancer stemness. Our RNA-seq and ChIRP-seq data indicate that Malat1 KO downregulates several immune evasion and stemness associated genes. Strikingly, Malat1 KO cells exhibit metastatic outgrowth when injected in T cells defective mice. Our single-cell RNA-seq cluster analysis and multi-color flow cytometry data show a greater proportion of T cells and reduce Neutrophils infiltration in KO mice which indicate that the immune microenvironment playing an important role in Malat1-dependent immune evasion. Mechanistically, loss of Malat1 is associated with reduced expression of Serpinb6b, which protects the tumor cells from cytotoxic killing by the T cells. Indeed, overexpression of Serpinb6b rescued the metastatic potential of Malat1 KO cells by protecting against cytotoxic T cells. Conclusions Collectively, our data indicate that targeting this novel cancer-cell-initiated domino effect within the immune system represents a new strategy to inhibit tumor metastatic reactivation. Trial Registration N/A Ethics Approval For all the animal studies in the present study, the study protocols were approved by the Institutional Animal Care and Use Committee(IACUC) of UT MD Anderson Cancer Center. Consent N/A References Arun G, Diermeier S, Akerman M, et al., Differentiation of mammary tumors and reduction in metastasis upon Malat1 lncRNA loss. Genes Dev 2016 Jan 1;30(1):34–51. Filippo G. Giancotti, mechanisms governing metastatic dormancy and reactivation. Cell 2013 Nov 7;155(4):750–764. Gao H, Chakraborty G, Lee-Lim AP, et al., The BMP inhibitor Coco reactivates breast cancer cells at lung metastatic sites. Cell 2012b;150:764–779. Gao H, Chakraborty G, Lee-Lim AP, et al., Forward genetic screens in mice uncover mediators and suppressors of metastatic reactivation. Proc Natl Acad Sci U S A 2014 Nov 18; 111(46): 16532–16537.

Published
2020

36. Prostate Epithelial Genes Define Docetaxel-Sensitive Prostate Cancer Molecular Subtype

Author

Won Sik Ham, Kwibok Choi, Nam Hoon Cho, Ji Eun Heo, Koon Ho Rha, Young Jun Moon, Won Sik Jang, Filippo G. Giancotti, Young Deuk Choi, and Hyunho Han

Subjects
Stromal cell, Biology, medicine.disease, Transcriptome, Androgen receptor, Prostate cancer, medicine.anatomical_structure, Docetaxel, Prostatic acid phosphatase, Antigen, Prostate, medicine, Cancer research, medicine.drug
Abstract

BACKGROUND & OBJECTIVESAnalysis of the transcriptomic landscape of prostate adenocarcinoma shows multidimensional gene expression variability. Understanding cancer transcriptome complexity can provide biological insight and therapeutic guidance. To avoid potential confounding factors, such as stromal contamination and stress-related material degradation, we utilized a set of genes expressed by prostate epithelial cells from single-cell transcriptome data of the human prostate gland.MATERIALS & METHODSAnalyzing publicly available bulk and single-cell RNA sequencing data, we defined 1,629 genes expressed by prostate epithelial cells. Consensus clustering and CIBERSORT deconvolution were used for class discovery and proportion estimate analysis. The Cancer Genome Atlas Prostate Adenocarcinoma (TCGA-PRAD) dataset served as a training set. The resulting clusters were analyzed in association with clinical, pathologic, and genomic characteristics and impact on survival.RESULTSTCGA-PRAD tumors were separated into four subtypes: A (30.0%), B (26.0%), C (14.7%), D (4.2%), and mixed (25.0%). Subtype A was characterized by low frequency of ETS-family fusions and high expression of KLK3, which encodes prostate-specific antigen (PSA). Subtype B showed the highest expression of ACP3, encoding PAP (prostatic acid phosphatase). Subtypes C and D were commonly associated with advanced T/N stages, high Gleason grades, and p53 or PIK3CA mutations. In silico drug-sensitivity screening suggested that subtype B is likely sensitive to docetaxel and paclitaxel. Serum PSA/PAP ratio was predictive of a radiographic response to docetaxel in metastatic castration-resistant prostate cancer patients.CONCLUSIONWe propose four prostate adenocarcinoma subtypes with distinct transcriptomic, genomic, and pathologic characteristics. PSA/PAP ratio in advanced cancer may aid in determining which patients would benefit from maximized androgen receptor inhibition or early use of antimicrotubule agents. Molecular subtypes and biomarkers must be validated in a prospective cohort study.

Published
2020
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38. Efficient Shot Detector: Lightweight Network Based on Deep Learning Using Feature Pyramid

Author

Sang-Hun Lee, Hyunho Han, and Chan-Soo Park

Subjects
Technology, Computational complexity theory, QH301-705.5, Computer science, QC1-999, Feature extraction, General Materials Science, Pyramid (image processing), Biology (General), QD1-999, Instrumentation, Fluid Flow and Transfer Processes, Pointwise, business.industry, Physics, Process Chemistry and Technology, Deep learning, Detector, General Engineering, object detection, Pattern recognition, Engineering (General). Civil engineering (General), EfficientNet, Object detection, Computer Science Applications, Chemistry, feature pyramid, Feature (computer vision), Artificial intelligence, TA1-2040, business, CNN, lightweight deep learning
Abstract

Convolutional-neural-network (CNN)-based methods are continuously used in various industries with the rapid development of deep learning technologies. However, an inference efficiency problem was reported in applications that require real-time performance, such as a mobile device. It is important to design a lightweight network that can be used in general-purpose environments such as mobile environments and GPU environments. In this study, we propose a lightweight network efficient shot detector (ESDet) based on deep training with small parameters. The feature extraction process was performed using depthwise and pointwise convolution to minimize the computational complexity of the proposed network. The subsequent layer was formed in a feature pyramid structure to ensure that the extracted features were robust to multiscale objects. The network was trained by defining a prior box optimized for the data set of each feature scale. We defined an ESDet-baseline with optimal parameters through experiments and expanded it by gradually increasing the input resolution for detection accuracy. ESDet training and evaluation was performed using the PASCAL VOC and MS COCO2017 Dataset. Moreover, the average precision (AP) evaluation index was used for quantitative evaluation of detection performance. Finally, superior detection efficiency was demonstrated through the experiment compared to the conventional detection method.

Published
2021
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39. Relationship between parental regulation of Internet game use and risk of Internet gaming disorder in children

Author

Hyunsuk Jeong, Hyunho Han, Bhang, Soo-young, Seung-Yup Lee, Lee Hae Kook, Yong-Sil Kweon, Jung Seok Choi, Sun Jin Jo, Hye Jung Son, Hyeon-Woo Yim, and Eunjin Kim

Subjects
03 medical and health sciences, 0302 clinical medicine, business.industry, Internet privacy, 030508 substance abuse, The Internet, 030212 general & internal medicine, 0305 other medical science, business, Psychology
Published
2017
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40. Improved YOLOv3 with duplex FPN for object detection based on deep learning

Author

Seokyong Shin, Hyunho Han, and Sang-Hun Lee

Subjects
Computer science, business.industry, Deep learning, Darknet, Duplex (telecommunications), 02 engineering and technology, Object detection, Education, 020204 information systems, 0202 electrical engineering, electronic engineering, information engineering, Object detector, 020201 artificial intelligence & image processing, Computer vision, Artificial intelligence, Electrical and Electronic Engineering, business
Abstract

YOLOv3 is a deep learning-based real-time object detector and is mainly used in applications such as video surveillance and autonomous vehicles. In this paper, we proposed an improved YOLOv3 (You Only Look Once version 3) applied Duplex FPN, which enhanced large object detection by utilizing low-level feature information. The conventional YOLOv3 improved the small object detection performance by applying FPN (Feature Pyramid Networks) structure to YOLOv2. However, YOLOv3 with an FPN structure specialized in detecting small objects, so it is difficult to detect large objects. Therefore, this paper proposed an improved YOLOv3 applied Duplex FPN, which can utilize low-level location information in high-level feature maps instead of the existing FPN structure of YOLOv3. This improved the detection accuracy of large objects. Also, an extra detection layer was added to the top-level feature map to prevent failure of detection of parts of large objects. Further, dimension clusters of each detection layer were reassigned to learn quickly how to accurately detect objects. The proposed method was compared and analyzed in the PASCAL VOC dataset. The experimental results showed that the bounding box accuracy of large objects improved owing to the Duplex FPN and extra detection layer, and the proposed method succeeded in detecting large objects that the existing YOLOv3 did not.

Published
2021
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41. The association between aggression and risk of Internet gaming disorder in Korean adolescents: the mediation effect of father-adolescent communication style

Author

Sun-Jin Jo, Eunjin Kim, Hyunho Han, Hyeon Woo Yim, Hyunsuk Jeong, Hye Jung Son, and Hae Kook Lee

Subjects
Male, Risk, Mediation (statistics), Adolescent, Addictive behavior, lcsh:Medicine, Structural equation modeling, Developmental psychology, Style (sociolinguistics), Cohort Studies, 03 medical and health sciences, 0302 clinical medicine, Republic of Korea, Medicine, Humans, Association (psychology), Father-Child Relations, Internet, business.industry, Aggression, Communication, lcsh:R, Mediation, General Medicine, medicine.disease, 030227 psychiatry, Behavior, Addictive, Cohort, Gambling, The Internet, Female, Original Article, medicine.symptom, business, 030217 neurology & neurosurgery
Abstract

Objectives Open and supportive communication between parents and children is known to reduce adolescents' delinquent behavior. Recently, the risk of Internet gaming disorder (IGD) has been increasing in adolescents. The purpose of this study was to investigate the mediating effects of parent-child communication styles on the relationship between adolescent aggressiveness and risk of IGD. Methods Participants in this study were 402 first-year students from 4 middle schools in Seoul who enrolled in the Internet user Cohort for Unbiased Recognition of gaming disorder in Early adolescence (iCURE) and completed baseline assessment in 2016. The structural equation model was constructed based on an aggression questionnaire, the Internet game use-elicited symptom screen, a mother-child communication inventory, and a father-child communication inventory. Results Adolescents' aggressiveness was found to be related to their risk of IGD. The father-child communication style mediated the relationship between aggression and risk of IGD. However, the mother-child communication style had no mediating effect. Conclusions Our findings suggest that fathers should make an effort to improve open and positive communication skills with their children, because the father-child communication style plays an important role in the relationship between adolescent aggressiveness and risk of IGD.

Published
2018

42. Abstract 1531: The Polycomb repressor complex 1 promotes recruitment of myeloid-derived suppressor cells and immune evasion during bone colonization in castration-resistant prostate cancer

Author

Goutam Chakraborty, Guangli Yang, Boyu Zhang, Wenjing Su, Ouathek Ouerfelli, Howard I. Scher, Hyunho Han, Jie Su, Bing Zhou, Neal Rosen, and Filippo G. Giancotti

Subjects
Cancer Research, Tumor microenvironment, medicine.medical_treatment, Repressor, Cancer, Immunotherapy, Biology, medicine.disease, Metastasis, Prostate cancer, Oncology, Cancer stem cell, medicine, Myeloid-derived Suppressor Cell, Cancer research
Abstract

The mechanisms that enable immune evasion at metastatic sites are poorly understood. We show that the Polycomb Repressor Complex-1 (PRC1) drives colonization of the bones and visceral organs in Double Negative (AR- NE-) Prostate Cancer (DNPC). In vivo genetic screening identifies the cytokine CCL2 as the top pro-metastatic gene induced by PRC1. Mechanistic studies show that CCL2 not only controls self-renewal and metastatic initiation but also governs the recruitment of M2-like TAMs and Tregs, thus creating a profoundly immune suppressive and proangiogenic microenvironment. Inhibition of PRC1 reverses these processes and cooperates with checkpoint immunotherapy to suppress multi-organ site metastasis. These results reveal a link between epigenetic regulation of cancer stem cells and molding of the tumor microenvironment and identify PRC1 as a potential therapeutic target in M-CRPC. Citation Format: Wenjing Su, Boyu Zhang, Hyunho Han, Goutam Chakraborty, Bing Zhou, Jie Su, Guangli Yang, Ouathek Ouerfelli, Neal Rosen, Howard I. Scher, Filippo G. Giancotti. The Polycomb repressor complex 1 promotes recruitment of myeloid-derived suppressor cells and immune evasion during bone colonization in castration-resistant prostate cancer [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2019; 2019 Mar 29-Apr 3; Atlanta, GA. Philadelphia (PA): AACR; Cancer Res 2019;79(13 Suppl):Abstract nr 1531.

Published
2019
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