Your search keyword '"Chiou, Jeng-Fong"' showing total 17 results

1. Effectiveness of Stereotactic Ablative Radiotherapy for Systemic Therapy Respondents with Inoperable Pulmonary Oligometastases and Oligoprogression.

Author

Ho, Chin-Beng, Tsai, Jo-Ting, Chen, Chun-You, Shiah, Her-Shyong, Chen, Hsuan-Yu, Ting, Lai-Lei, Kuo, Chia-Chun, Lai, I-Chun, Lai, Hsin-Yi, Chung, Chi-Li, Lee, Kai-Ling, Tzeng, Huey-En, Lee, Kuen-Haur, Lee, Hsin-Lun, Chen, Shang-Wen, and Chiou, Jeng-Fong

Subjects

STEREOTACTIC radiotherapy, PROGNOSIS, LUNG tumors, RADIATION pneumonitis, PROGRESSION-free survival

Abstract

Stereotactic ablative radiotherapy (SABR) may improve survival in patients with inoperable pulmonary oligometastases. However, the impact of pulmonary oligometastatic status after systemic therapy on SABR outcomes remains unclear. Hence, we investigated the outcomes of SABR in 45 patients with 77 lung tumors and the prognostic value of pulmonary oligoprogression. Eligibility criteria were pulmonary oligometastases (defined as ≤5 metastatic lung tumors), controlled extrapulmonary disease (EPD) after front-line systemic therapy, SABR as primary local treatment for inoperable pulmonary metastases, and consecutive imaging follow-up. Oligometastatic lung tumor was classified into controlled or oligoprogressive status. Overall survival (OS), in-field progression-free survival (IFPFS), out-field progression-free survival (OFPFS), and prognostic variables were evaluated. With 21.8 months median follow-up, the median OS, IFPFS, and OFPFS were 28.3, not reached, and 6.5 months, respectively. Two-year OS, IFPFS, and OFPFS rates were 56.0%, 74.2%, and 17.3%, respectively. Oligoprogressive status (p = 0.003), disease-free interval < 24 months (p = 0.041), and biologically effective dose (BED10) < 100 Gy (p = 0.006) were independently associated with inferior OS. BED10 ≥ 100 Gy (p = 0.029) was independently correlated with longer IFPFS. Oligoprogressive status (p = 0.017) and EPD (p = 0.019) were significantly associated with inferior OFPFS. Grade ≥ 2 radiation pneumonitis occurred in four (8.9%) patients. Conclusively, SABR with BED10 ≥ 100 Gy could provide substantial in-field tumor control and longer OS for systemic therapy respondents with inoperable pulmonary oligometastases. Oligoprogressive lung tumors exhibited a higher risk of out-field treatment failure and shorter OS. Hence, systemic therapy should be tailored for patients with oligoprogression to reduce the risk of out-field treatment failure. However, in the absence of effective systemic therapy, SABR is a reasonable alternative to reduce resistant tumor burden. [ABSTRACT FROM AUTHOR]

Published

2023

2. Feasibility and Toxicity of Interval-Compressed Chemotherapy in Asian Children and Young Adults with Sarcoma.

Author

Huang, Jia-Hui, Chen, Shu-Huey, Liao, Yu-Mei, Kao, Yu-Chien, Ho, Wan-Ling, Chang, Hsi, Tsai, Min-Lan, Lee, Hsin-Lun, Kuo, Chia-Chun, Tseng, Sung-Hui, Chang, Chia-Yau, Hsieh, Kevin Li-Chun, Lu, Long-Sheng, Chen, Yin-Ju, Chiou, Jeng-Fong, Hsieh, Tsung-Han, Liu, Yun-Ru, Hsu, Wayne, Li, Wei-Tang, and Wu, Yu-Chung

Subjects

YOUNG adults, CARBOPLATIN, ASIANS, SCHWANNOMAS, SARCOMA, EWING'S sarcoma, PLATELET count, FEVER

Abstract

Simple Summary: Interval-compressed chemotherapy was evaluated in Asian children and young adults with sarcomas to assess the feasibility of this treatment strategy. Ultimately, the goal is to improve survival in this group of individuals with high-risk malignancies without increasing short-term or long-term toxicities. The feasibility of this strategy in Asian patients with sarcomas needed to be established prior to evaluating the efficacy of this approach in a prospective trial. Twelve Asian patients with sarcoma received interval-compressed (ic-) chemotherapy scheduled every 14 days with a regimen of vincristine (2 mg/m2), doxorubicin (75 mg/m2), and cyclophosphamide (1200–2200 mg/m2) (VDC) alternating with a regimen of ifosfamide (9000 mg/m2) and etoposide (500 mg/m2) (IE), with filgrastim (5–10 mcg/kg/day) between cycles. Carboplatin (800 mg/m2) was added for CIC-rearranged sarcoma. The patients were treated with 129 cycles of ic-VDC/IE with a median interval of 19 days (interquartile range [IQR], 15–24 days. Median nadirs (IQR) were neutrophil count, 134 (30–396) × 106/L at day 11 (10–12), recovery by day 15 (14–17) and platelet count, 35 (23–83) × 109/L at day 11 (10–13), recovery by day 17 (14–21). Fever and bacteremia were observed in 36% and 8% of cycles, respectively. The diagnoses were Ewing sarcoma (6), rhabdomyosarcoma (3), myoepithelial carcinoma (1), malignant peripheral nerve sheath tumor (1), and CIC-DUX4 Sarcoma (1). Seven of the nine patients with measurable tumors responded (one CR and six PR). Interval-compressed chemotherapy is feasible in the treatment of Asian children and young adults with sarcomas. [ABSTRACT FROM AUTHOR]

Published

2023

3. Recent Advances in Metal-Based NanoEnhancers for Particle Therapy.

Author

Chuang, Yao-Chen, Wu, Ping-Hsiu, Shen, Yao-An, Kuo, Chia-Chun, Wang, Wei-Jun, Chen, Yu-Chen, Lee, Hsin-Lun, and Chiou, Jeng-Fong

Subjects

HEALTH facilities, PROTON therapy, RADIATION damage, X-ray absorption, CANCER treatment, PHOTON beams

Abstract

Radiotherapy is one of the most common therapeutic regimens for cancer treatment. Over the past decade, proton therapy (PT) has emerged as an advanced type of radiotherapy (RT) that uses proton beams instead of conventional photon RT. Both PT and carbon-ion beam therapy (CIBT) exhibit excellent therapeutic results because of the physical characteristics of the resulting Bragg peaks, which has been exploited for cancer treatment in medical centers worldwide. Although particle therapies show significant advantages to photon RT by minimizing the radiation damage to normal tissue after the tumors, they still cause damage to normal tissue before the tumor. Since the physical mechanisms are different from particle therapy and photon RT, efforts have been made to ameliorate these effects by combining nanomaterials and particle therapies to improve tumor targeting by concentrating the radiation effects. Metallic nanoparticles (MNPs) exhibit many unique properties, such as strong X-ray absorption cross-sections and catalytic activity, and they are considered nano-radioenhancers (NREs) for RT. In this review, we systematically summarize the putative mechanisms involved in NRE-induced radioenhancement in particle therapy and the experimental results in in vitro and in vivo models. We also discuss the potential of translating preclinical metal-based NP-enhanced particle therapy studies into clinical practice using examples of several metal-based NREs, such as SPION, Abraxane, AGuIX, and NBTXR3. Furthermore, the future challenges and development of NREs for PT are presented for clinical translation. Finally, we propose a roadmap to pursue future studies to strengthen the interplay of particle therapy and nanomedicine. [ABSTRACT FROM AUTHOR]

Published

2023

4. Molecularly Targeted Photothermal Ablation of Epidermal Growth Factor Receptor-Expressing Cancer Cells with a Polypyrrole–Iron Oxide–Afatinib Nanocomposite.

Author

Rethi, Lekshmi, Mutalik, Chinmaya, Rethi, Lekha, Chiang, Wei-Hung, Lee, Hsin-Lun, Pan, Wen-Yu, Yang, Tze-Sen, Chiou, Jeng-Fong, Chen, Yin-Ju, Chuang, Er-Yuan, and Lu, Long-Sheng

Subjects

THERMOTHERAPY, NEAR infrared spectroscopy, PHOTOTHERAPY, EPIDERMAL growth factor receptors, CELL membranes, PROTEIN kinase inhibitors, IRON oxide nanoparticles, APOPTOSIS, AFATINIB, TREATMENT effectiveness, CELL motility, POLYMERS, CELL lines, REACTIVE oxygen species, ABLATION techniques, IRON compounds, NANOPARTICLES

Abstract

Simple Summary: In this manuscript, we describe the design and synthesis of a nanocomposite containing afatinib, polypyrrole, and iron oxide (PIA-NC) to molecularly target epidermal growth factor receptor (EGFR)-overexpressing cancer cells for photothermal conversion. In addition to physical and chemical characterization, we also showed that PIA-NC induces selective reactive oxygen species surge and apoptosis in response to sublethal near-infrared light only in EGFR-overexpressing cancer cells, not in EGFR-negative fibroblasts. The work demonstrates the feasibility of photothermal therapy with cellular precision. Near-infrared–photothermal therapy (NIR-PTT) is a potential modality for cancer treatment. Directing photothermal effects specifically to cancer cells may enhance the therapeutic index for the best treatment outcome. While epithelial growth factor receptor (EGFR) is commonly overexpressed/genetically altered in human malignancy, it remains unknown whether targeting EGFR with tyrosine kinase inhibitor (TKI)-conjugated nanoparticles may direct NIR-PTT to cancers with cellular precision. In the present study, we tested this possibility through the fabrication of a polypyrrole–iron oxide–afatinib nanocomposite (PIA-NC). In the PIA-NC, a biocompatible and photothermally conductive polymer (polypyrrole) was conjugated to a TKI (afatinib) that binds to overexpressed wild-type EGFR without overt cytotoxicity. A Fenton catalyst (iron oxide) was further encapsulated in the NC to drive the intracellular ROS surge upon heat activation. Diverse physical and chemical characterization experiments were conducted. Particle internalization, cytotoxicity, ROS production, and apoptosis in EGFR-positive and -negative cell lines were investigated in the presence and absence of NIR. We found that the PIA-NCs were stable with a size of 243 nm and a zeta potential of +35 mV. These PIA-NCs were readily internalized close to the cell membrane by all types of cells used in the study. The Fourier transform infrared spectra showed 3295 cm−1 peaks; substantial O–H stretching was seen, with significant C=C stretching at 1637 cm−1; and a modest appearance of C–O–H bending at 1444 cm−1 confirmed the chemical conjugation of afatinib but not iron oxide to the NC. At a NIR-PTT energy level that has a minimal cytotoxic effect, PIA-NC significantly sensitizes EGFR-overexpressing A549 lung cancer cells to NIR-PTT-induced cytotoxicity at a rate of 70%, but in EGFR-negative 3T3 fibroblasts the rate was 30%. Within 1 min of NIR-PTT, a surge of intracellular ROS was found in PIA-NC-treated A549 cells. This was followed by early induction of cellular apoptosis for 54 ± 0.081% of A549 cells. The number of viable cells was less than a quarter of a percent. Viability levels of A549 cells that had been treated with NIR or PIA were only 50 ± 0.216% and 80 ± 0.216%, respectively. Only 10 ± 0.816% of NIH3T3 cells had undergone necrosis, meaning that 90 ± 0.124% were alive. Viability levels were 65 ± 0.081% and 81 ± 0.2%, respectively, when only NIR and PIA were used. PIA binding was effective against A549 cells but not against NIH3T3 cells. The outcome revealed that higher levels of NC + NIR exposure caused cancer cells to produce more ROS. In summary, our findings proved that a molecularly targeted NC provides an orchestrated platform for cancer cell-specific delivery of NIR-PTT. The geometric proximity design indicates a novel approach to minimizing the off-target biological effects of NIR-PTT. The potential of PIA-NC to be further developed into real-world application warrants further investigation. [ABSTRACT FROM AUTHOR]

Published

2022

5. Retrospective Analysis for Dose Reduction to Organs at Risk with New Personalized Breast Holder (PERSBRA) in Left Breast IMRT.

Author

Chen, Chiu-Ping, Chen, Tung-Ho, Chiou, Jeng-Fong, Chen, Yi-Ju, Kuo, Chia-Chun, Tseng, Kuo-Hsiung, Chung, Meng-Yun, Chen, Chun-You, Wu, Jeng-You, Lu, Long-Sheng, and Hsu, Shih-Ming

Subjects

BREAST, INTENSITY modulated radiotherapy, LUMPECTOMY, RADIATION doses, CARDIAC patients, CANCER treatment

Abstract

This study evaluated dose differences in normal organs at risk, such as the lungs, heart, left anterior descending artery (LAD), right coronary artery, left ventricle, and right breast under personalized breast holder (PERSBRA), when using intensity-modulated radiation therapy (IMRT). This study evaluated the radiation protection offered by PERSBRA in left breast cancer radiation therapy. Here, we retrospectively collected data from 24 patients with left breast cancer who underwent breast-conserving surgery as well as IMRT radiotherapy. We compared the dose differences in target coverage and organs at risk with and without PERSBRA. For target coverage, tumor prescribed dose 95% coverage, conformity index, and homogeneity index were evaluated. For organs at risk, we compared the mean heart dose, mean left ventricle dose, LAD maximum and mean dose, mean left lung receiving 20 Gy, 10 Gy, and 5 Gy of left lung volume, maximum and mean coronary artery of the right, maximum of right breast, and mean dose. Good target coverage was achieved with and without PERSBRA. When PERSBRA was used with IMRT, the mean dose of the heart decreased by 42%, the maximum dose of LAD decreased by 26.4%, and the mean dose of LAD decreased by 47.0%. The mean dose of the left ventricle decreased by 54.1%, the volume (V20) of the left lung that received 20 Gy decreased by 22.8%, the volume (V10) of the left lung that received 10 Gy decreased by 19.8%, the volume (V5) of the left lung that received 5 Gy decreased by 15.7%, and the mean dose of the left lung decreased by 23.3%. Using PERSBRA with IMRT greatly decreases the dose to organs at risk (left lung, heart, left ventricle, and LAD). This study found that PERSBRA with IMRT can achieve results similar to deep inspiration breath-hold radiotherapy (DIBH) in terms of reducing the heart radiation dose and the risk of developing heart disease in patients with left breast cancer who cannot undergo DIBH. [ABSTRACT FROM AUTHOR]

Published

2022

6. Skin Surface Dose for Whole Breast Radiotherapy Using Personalized Breast Holder: Comparison with Various Radiotherapy Techniques and Clinical Experiences.

Author

Chen, Chiu-Ping, Lin, Chi-Yeh, Kuo, Chia-Chun, Chen, Tung-Ho, Lin, Shao-Chen, Tseng, Kuo-Hsiung, Cheng, Hao-Wen, Chao, Hsing-Lung, Yen, Sang-Hue, Lin, Ruo-Yu, Feng, Chen-Ju, Lu, Long-Sheng, Chiou, Jeng-Fong, and Hsu, Shih-Ming

Subjects

RADIATION therapy equipment, STATISTICS, MANN Whitney U Test, RADIATION doses, DESCRIPTIVE statistics, RADIOTHERAPY, DATA analysis software, DATA analysis, BREAST tumors

Abstract

Simple Summary: Breast immobilization with personalized breast holder (PERSBRA) is a promising approach to reduce the toxicity in the lungs and heart during whole breast radiotherapy. In this study, we designed PERSBRA with three different mesh sizes (large, fine and solid) and applied them on a Rando phantom. Hybrid, intensity modulated radiation therapy (IMRT), and volumetric modulated arc therapy (VMAT) techniques were used to deliver a prescribed dose. The dose measurement with EBT3 film and TLD were taken on Rando phantom with no PERSBRA, large mesh, fine mesh, and solid PERSBRA for tumor doses and surface doses. This innovative PERSBRA provides another radiotherapy option for patients with left breast cancer. Purpose: Breast immobilization with personalized breast holder (PERSBRA) is a promising approach for normal organ protection during whole breast radiotherapy. The aim of this study is to evaluate the skin surface dose for breast radiotherapy with PERSBRA using different radiotherapy techniques. Materials and methods: We designed PERSBRA with three different mesh sizes (large, fine and solid) and applied them on an anthropomorphic(Rando) phantom. Treatment planning was generated using hybrid, intensity-modulated radiotherapy (IMRT) and volumetric-modulated arc therapy (VMAT) techniques to deliver a prescribed dose of 5000 cGy in 25 fractions accordingly. Dose measurement with EBT3 film and TLD were taken on Rando phantom without PERSBRA, large mesh, fine mesh and solid PERSBRA for (a) tumor doses, (b) surface doses for medial field and lateral field irradiation undergoing hybrid, IMRT, VMAT techniques. Results: The tumor dose deviation was less than five percent between the measured doses of the EBT3 film and the TLD among the different techniques. The application of a PERSBRA was associated with a higher dose of the skin surface. A large mesh size of PERSBRA was associated with a lower surface dose. The findings were consistent among hybrid, IMRT, or VMAT techniques. Conclusions: Breast immobilization with PERSBRA can reduce heart toxicity but leads to a build-up of skin surface doses, which can be improved with a larger mesh design for common radiotherapy techniques. [ABSTRACT FROM AUTHOR]

Published

2022

7. Recent Advances in Gold Nanomaterials for Photothermal Therapy.

Author

Chuang, Yao-Chen, Lee, Hsin-Lun, Chiou, Jeng-Fong, and Lo, Leu-Wei

Subjects

NANOSTRUCTURED materials, GOLD nanoparticles, PHOTOTHERMAL conversion, TUMOR treatment, TREATMENT effectiveness, CANCER treatment

Abstract

Gold nanoparticle (AuNPs)-mediated photothermal therapy (PTT) has attracted increasing attention both in laboratory research and clinical applications. Due to its easily-tuned properties of irradiation light and inside-out hyperthermia ability, it has demonstrated clear advantages in cancer therapy over conventional thermal ablation. Despite this great advancement, the therapeutic efficacy of AuNPs mediated PTT in tumor treatment remains compromised by several obstacles, including low photothermal conversion efficiency, tissue penetration limitation of excitation light, and inherent non-specificity. In view of the rapid development of AuNPs mediated PTT, we present an in-depth review of major breakthroughs in the advanced development of gold nanomaterials for PTT, with emphasis on those from 2010 to date. In particular, the current state of knowledge for AuNPs based photothermal agents within a paradigm of key structure-optical property relationships is presented in order to provide guidance for the design of novel AuNP based photothermal agents to meet necessary functional requirements in specific applications. Furthermore, potential challenges and future development of AuNP mediated PTT are also elucidated for clinical translation. It is expected that AuNP mediated PTT will soon constitute a markedly promising avenue in the treatment of cancer. [ABSTRACT FROM AUTHOR]

Published

2022

8. Microtube Array Membrane Hollow Fiber Assay (MTAM-HFA)—An Accurate and Rapid Potential Companion Diagnostic and Pharmacological Interrogation Solution for Cancer Immunotherapy (PD-1/PD-L1).

Author

Huang, Wan-Ting, Yun, Tsao, Chew, Chee-Ho, Chen, Amanda, Wei, Po-Li, Lee, Kang-Yun, Lee, Hsin-Lun, Feng, Po-Hao, Chiou, Jeng-Fong, Chen, Ching-Mei, and Chen, Chien-Chung

Subjects

CYTOTOXIC T cells, HOLLOW fibers, MONONUCLEAR leukocytes, PROGRAMMED cell death 1 receptors, PROGRAMMED death-ligand 1, IMMUNOTHERAPY

Abstract

Immunotherapy is one of the most promising forms of cancer treatment. In particular, immune checkpoint blockers (ICBs) represent some of the leading candidates which many drug developers have heavily invested in. During pre-clinical development and prior to human clinical trials, animal tests are a critical component for determining the safety and efficacy of newly developed ICBs for cancer treatment. In this study, we strive to demonstrate the feasibility of using hollow fiber assay microtube array membrane (MTAM-HFA) in the screening of anti-cancer ICBs. The MTAM-HFA process was carried out by encapsulating peripheral blood mononuclear cells (PBMCs) and the target cancer cells (cell lines or primary cells) and subcutaneously implanting them into Balb/C mice. At predetermined time points combination regimens of PD-1/PD-L1+ were administered accordingly and at a predetermined time point, the MTAMs were retrieved, and cell viability assays were carried out. The outcomes of the MTAM-HFA were compared against the clinical outcome of patients. Clinical comparison demonstrated excellent correlation between the screening outcome of MTAM-HFA of PD-1/PD-L1+ combination therapy and the clinical outcome of the lung cancer patients. Basic cell studies revealed that the utilization of MTAM-HFA in PD-1/PD-L1+ combination therapy revealed enhanced T-cell activity upon the administration of the PD-1/PD-L1 drug; thereby resulting in the reduction of tumor cell viability by up to 70%, and the cytotoxic effects by 82%. The outcome was echoed in the in vivo cell studies. This suggested that the MTAM-HFA system is suitable for use in PD-1/PD-L1+ screening and the accuracy, rapidity and cost effectiveness made it extremely suitable for application as a companion diagnostic system in both personalized medicine for cancer treatment and could potentially be applied to screen for candidate compounds in the development of next generation PD-1/PD-L1+ combination therapies. [ABSTRACT FROM AUTHOR]

Published

2022

9. Hepatic Reirradiation for Patients with Recurrent Hepatocellular Carcinoma.

Author

Huang, Yaoru, Chen, Po-Yung, Cheng, Tzu-Yen, Chiou, Jeng-Fong, and Yamasaki, Takahiro

Subjects

HEPATOCELLULAR carcinoma, CHEMOEMBOLIZATION, CATHETER ablation, TREATMENT effectiveness, PORTAL vein, HEPATIC portal system, INTRAHEPATIC bile ducts

Abstract

Featured Application: Hepatocellular carcinoma (HCC) may easily recur because of multifocal carcinogenesis. For recurrent HCC, good local control indicates better survival. For HCC-contradicting local therapies such as surgery, transarterial chemoembolization and radiofrequency ablation, several studies have discussed the feasibility of reirradiation. This study investigated the treatment outcomes of reirradiation and discovered better local control may still prolong survival after reirradiation for recurrent HCC. This may suggest a new treatment approach for treating HCC. For treating hepatocellular carcinoma (HCC), local therapies and surgery, including liver transplant, are the first line treatment options; however, several contraindications limit their clinical use. The improvement of radiotherapy (RT) established RT in treating HCC contraindicated against local therapies, including transarterial chemoembolization and radiofrequency ablation. For HCC that recurs after RT and still contradicts against local therapies, there is a need to investigate the use of reirradiation. This study recruited patients receiving two courses of RT for recurrent HCC between January 2007 and December 2019. The result suggested that patients who experienced tumor regression after reirradiation had better survival over those with a stable form of the disease, with the mean overall survival (OS) as 30.0 and 4.0 months, respectively (p < 0.001). The analysis also revealed that systemic therapy had no benefit on both the OS and controlling distant metastasis; the result was limited to a small study number and diversity of drugs. Considering systemic therapy and portal vein tumor thrombosis, which are commonly viewed to affect prognosis, multivariate analysis suggested that the Child–Pugh score and local control were the only two independent factors for the OS, with p = 0.017 and p = 0.028, respectively. Our findings suggested that reirradiation could be the choice for treating recurrent HCC. [ABSTRACT FROM AUTHOR]

Published

2021

10. Nucleus Near-Infrared (nNIR) Irradiation of Single A549 Cells Induces DNA Damage and Activates EGFR Leading to Mitochondrial Fission.

Author

Gbetuwa, Momoh, Lu, Long-Sheng, Wang, Tsung-Jen, Chen, Yin-Ju, Chiou, Jeng-Fong, Su, Tai-Yuan, and Yang, Tzu-Sen

Subjects

DNA damage, EPIDERMAL growth factor, EPIDERMAL growth factor receptors, CELL nuclei, MITOCHONDRIA

Abstract

There has been great interest in identifying the biological substrate for light-cell interaction and their relations to cancer treatment. In this study, a near-infrared (NIR) laser is focused into the nucleus (nNIR) or cytoplasm (cNIR) of a single living cell by a high numerical aperture condenser to dissect the novel role of cell nucleus in mediating NIR effects on mitochondrial dynamics of A549 non-small cell lung cancer cells. Our analysis showed that nNIR, but not cNIR, triggered mitochondrial fission in 10 min. In contrast, the fission/fusion balance of mitochondria directly exposed to cNIR does not change. While the same phenomenon is also triggered by single molecular interactions between epidermal growth factor (EGF) and its receptor EGFR, pharmacological studies with cetuximab, PD153035, and caffeine suggest EGF signaling crosstalk to DNA damaging response to mediate rapid mitochondrial fission as a result of nNIR irradiation. These results suggest that nuclear DNA integrity is a novel biological target for cellular response to NIR. [ABSTRACT FROM AUTHOR]

Published

2022

11. Humoral Immunogenicity and Reactogenicity of the Standard ChAdOx1 nCoV-19 Vaccination in Taiwan.

Author

Chang, Jer-Hwa, Chiou, Jeng-Fong, Hung, Ching-Sheng, Liu, Ming-Che, Chang, Hui-Wen, Hong, Shiao-Ya, Wang, Cheng-Yi, Lin, Yi-Ling, Hsieh, Yi-Chen, Chung, Chi-Li, Su, Ying-Shih, Hsiao, Shu-Tai Shen, Liu, Doresses, Liang, Jian-Jong, Liao, Chun-Che, Chang, Chih-Shin, Lai, Kevin Shu-Leung, Chuang, Han-Chuan, Chien, Ko-Ling, and Wu, Wei-Ciao

Subjects

IMMUNE response, VACCINATION, ASIANS, PLATELET count, HUMORAL immunity

Abstract

Background: The ChAdOx1 nCoV-19 vaccine has been widely administered against SARS-CoV-2 infection; however, data regarding its immunogenicity, reactogenicity, and potential differences in responses among Asian populations remain scarce. Methods: 270 participants without prior COVID-19 were enrolled to receive ChAdOx1 nCoV-19 vaccination with a prime–boost interval of 8–9 weeks. Their specific SARS-CoV-2 antibodies, neutralizing antibody titers (NT50), platelet counts, and D-dimer levels were analyzed before and after vaccination. Results: The seroconversion rates of anti-RBD and anti-spike IgG at day 28 after a boost vaccination (BD28) were 100% and 95.19%, respectively. Anti-RBD and anti-spike IgG levels were highly correlated (r = 0.7891), which were 172.9 ± 170.4 and 179.3 ± 76.88 BAU/mL at BD28, respectively. The geometric mean concentrations (GMCs) of NT50 for all participants increased to 132.9 IU/mL (95% CI 120.0–147.1) at BD28 and were highly correlated with anti-RBD and anti-spike IgG levels (r = 0.8248 and 0.7474, respectively). Body weight index was statistically significantly associated with anti-RBD IgG levels (p = 0.035), while female recipients had higher anti-spike IgG levels (p = 0.038). The GMCs of NT50 declined with age (p = 0.0163) and were significantly different across age groups (159.7 IU/mL for 20–29 years, 99.4 IU/mL for ≥50 years, p = 0.0026). Injection-site pain, fever, and fatigue were the major reactogenicity, which were more pronounced after prime vaccination and in younger participants (<50 years). Platelet counts decreased and D-dimer levels increased after vaccination but were not clinically relevant. No serious adverse events or deaths were observed. Conclusion: The vaccine is well-tolerated and elicited robust humoral immunity against SARS-CoV-2 after standard prime–boost vaccination in Taiwanese recipients. [ABSTRACT FROM AUTHOR]

Published

2022

12. A Few-Shot Learning Approach Assists in the Prognosis Prediction of Magnetic Resonance-Guided Focused Ultrasound for the Local Control of Bone Metastatic Lesions.

Author

Hsu, Fang-Chi, Lee, Hsin-Lun, Chen, Yin-Ju, Shen, Yao-An, Tsai, Yi-Chieh, Wu, Meng-Huang, Kuo, Chia-Chun, Lu, Long-Sheng, Yeh, Shauh-Der, Huang, Wen-Sheng, Shen, Chia-Ning, and Chiou, Jeng-Fong

Subjects

CYTOKINES, INTERLEUKINS, MAGNETIC resonance imaging, BONE tumors, LEARNING strategies, PRE-tests & post-tests, BONE metastasis, DESCRIPTIVE statistics, PHILOSOPHY of education, ULTRASONIC therapy, LOGISTIC regression analysis, VASCULAR endothelial growth factors

Abstract

Simple Summary: We report a local control prediction model for patients undergoing MRgFUS ablation, and provide promising guidance for clinicians to identify a suitable treatment strategy for bone metastatic lesions. We propose a few-shot learning approach to establish the quick prediction of clinical and radiographic responses. On the basis of demographic data, pre-/post-treatment immune-related cytokine change, and MRI imaging, the most suitable parameters were selected to assess potential treatment outcomes during the acute inflammatory stages within 24 h. Traditional logistic regression and few-shot learning models were compared to identify the best model on an independent test. The best predictive few-shot learning model (accuracy of 85.2%, sensitivity of 88.6%, and AUC of 0.95) was achieved by combining the clinical features with the levels of significant cytokines IL-6, IL-13, IP-10, and eotaxin. Magnetic resonance-guided focused ultrasound surgery (MRgFUS) constitutes a noninvasive treatment strategy to ablate deep-seated bone metastases. However, limited evidence suggests that, although cytokines are influenced by thermal necrosis, there is still no cytokine threshold for clinical responses. A prediction model to approximate the postablation immune status on the basis of circulating cytokine activation is thus needed. IL-6 and IP-10, which are proinflammatory cytokines, decreased significantly during the acute phase. Wound-healing cytokines such as VEGF and PDGF increased after ablation, but the increase was not statistically significant. In this phase, IL-6, IL-13, IP-10, and eotaxin expression levels diminished the ongoing inflammatory progression in the treated sites. These cytokine changes also correlated with the response rate of primary tumor control after acute periods. The few-shot learning algorithm was applied to test the correlation between cytokine levels and local control (p = 0.036). The best-fitted model included IL-6, IL-13, IP-10, and eotaxin as cytokine parameters from the few-shot selection, and had an accuracy of 85.2%, sensitivity of 88.6%, and AUC of 0.95. The acceptable usage of this model may help predict the acute-phase prognosis of a patient with painful bone metastasis who underwent local MRgFUS. The application of machine learning in bone metastasis is equivalent or better than the current logistic regression. [ABSTRACT FROM AUTHOR]

Published

2022

13. Ex Vivo Expanded Circulating Tumor Cells for Clinical Anti-Cancer Drug Prediction in Patients with Head and Neck Cancer.

Author

Lin, Kuan-Chou, Ting, Lai-Lei, Chang, Chia-Lun, Lu, Long-Sheng, Lee, Hsin-Lun, Hsu, Fang-Chi, Chiou, Jeng-Fong, Wang, Peng-Yuan, Burnouf, Thierry, Ho, Dennis Chun-Yu, Yang, Kai-Chiang, Chen, Chang-Yu, Chen, Chu-Huang, Wu, Ching-Zong, and Chen, Yin-Ju

Subjects

HEAD tumors, DRUG efficacy, TREATMENT effectiveness, CISPLATIN, CELL lines, PREDICTION models, BODY fluid examination, NECK tumors, EVALUATION

Abstract

Simple Summary: The conventional methods that seek to predict clinical treatment response are based on the number of circulating tumor cells (CTCs) present in liquid biopsies or genetic profiling of extracted CTCs. This paper presents a novel process by which CTCs can be extracted from blood samples taken from head and neck cancer patients and then expanded ex vivo to form organoids that can be tested with a panel of anti-cancer treatments. The resulting drug sensitivity profiles derived from cisplatin treatment of organoids were subsequently found to correlate with clinical treatment response to cisplatin in patients. CTCs extracted from liquid biopsies for ex vivo expansion negates the need for complicated and potentially risky biopsies of tumor material, thereby supporting the application of this procedure for checkups and treatment monitoring. The advanced-stage head and neck cancer (HNC) patients respond poorly to platinum-based treatments. Thus, a reliable pretreatment method for evaluating platinum treatment response would improve therapeutic efficiency and outcomes. This study describes a novel strategy to predict clinical drug responses in HNC patients by using eSelect, a lab-developed biomimetic cell culture system, which enables us to perform ex vivo expansion and drug sensitivity profiling of circulating tumor cells (CTCs). Forty liquid biopsies were collected from HNC patients, and the CTCs were expanded ex vivo using the eSelect system within four weeks. Immunofluorescence staining confirmed that the CTC-derived organoids were positive for EpCAM and negative for CD45. Two illustrative cases present the potential of this strategy for evaluating treatment response. The statistical analysis confirmed that drug sensitivity in CTC-derived organoids was associated with a clinical response. The multivariant logistic regression model predicted that the treatment accuracy of chemotherapy responses achieved 93.75%, and the area under the curves (AUCs) of prediction models was 0.8841 in the whole dataset and 0.9167 in cisplatin specific dataset. In summary, cisplatin sensitivity profiles of patient-derived CTCs expanded ex vivo correlate with a clinical response to cisplatin treatment, and this can potentially underpin predictive assays to guide HNC treatments. [ABSTRACT FROM AUTHOR]

Published

2021

14. Patient-Derived Tumor Chemosensitization of GKB202, an Antrodia Cinnamomea Mycelium-Derived Bioactive Compound.

Author

Li, Tsung-Ju, Lin, Ting-Wei, Wu, Shih-Pei, Chu, Hsin-Tung, Kuo, Yu-Hsuan, Chiou, Jeng-Fong, Lu, Long-Sheng, and Chen, Chin-Chu

Subjects

BIOACTIVE compounds, CHEMOSENSITIZERS, COLORECTAL cancer, CANCER-related mortality

Abstract

Oral cancers, hepatocellular carcinoma, and colorectal cancers are the three most common cancers, leading to 18,000 cases of cancer-related mortality in Taiwan per year. To bridge the gap towards clinical translation, we developed a circulating tumor cell (CTC) organoid culture workflow that efficiently expands CTC from patients to test Antrodia Cinnamomea mycelium-derived bioactive compounds. Three ACM-derived bioactive compounds were evaluated for tumor chemosensitization characteristics. Significant and consistent cytotoxic/5-FU sensitizing effects of GKB202 were found on 8 different patient-derived tumors. Acute toxicity profile and hepatic metabolism of GKB202 in rats suggest GKB202 is rapidly cleared by liver and is well tolerated up to the dose of 20 mg/kg. This comprehensive study provides new evidence that liquid fermentation of Antrodia cinnamomea mycelium (ACM) contains bioactive compounds that lead to effective control of CTC, especially when combined with 5-FU. Together, these data suggest ACM-derived GKB202 may be considered for further clinical investigation in the context of 5-FU-based combination therapy. [ABSTRACT FROM AUTHOR]

Published

2021

15. Ex Vivo Expansion and Drug Sensitivity Profiling of Circulating Tumor Cells from Patients with Small Cell Lung Cancer.

Author

Lee, Hsin-Lun, Chiou, Jeng-Fong, Wang, Peng-Yuan, Lu, Long-Sheng, Shen, Chia-Ning, Hsu, Han-Lin, Burnouf, Thierry, Ting, Lai-Lei, Chou, Pai-Chien, Chung, Chi-Li, Lee, Kai-Ling, Shiah, Her-Shyong, Liu, Yen-Lin, and Chen, Yin-Ju

Subjects

*PROTEIN metabolism, *BIOPSY, *CANCER patients, *CELL lines, *DECISION making, *DRUG resistance in cancer cells, *DRUG design, *CLINICAL drug trials, *FLUORESCENT antibody technique, *GENE expression, *LUNG tumors, *SURVIVAL, *TUMOR markers, *SMALL cell carcinoma

Abstract

Simple Summary: Small cell lung cancer (SCLC) is an overly aggressive cancer characterized by rapid growth, early metastatic spread, and consequently reducing overall survival. As cancer manifestations can differ uniquely between various types, the rapid proliferation of circulating tumor cells (CTC) originating from SCLC was an adequate sample resource to aid the headway in our drug screening technique. With biomarker detection of liquid biopsy as an emerging tool to assist decision-making in personalized cancer pharmacotherapy. In this study, we developed a rapid and reproducible system for preclinical drug testing via the use of a unique CTCs expansion protocol. The expanded CTCs from SCLC formed multiple types of tumorsphere structures and expressed SCLC-specific tumor markers. The drug sensitivity assessment gathered from in vitro expansion of CTCs was able to generate positive clinical therapeutic outcomes. Thus, SCLC patient-derived CTC spheroids are a useful resource for biomarker development and drug sensitivity assessment providing "real-world" therapeutic response circumstances. Small cell lung cancer (SCLC) represents one of the most aggressive malignancies among cancer types. Not only tumor sample availability is limited, but also the ability for tumor cells to rapidly acquire drug resistance are the rate-limiting bottlenecks for overall survival in current clinical settings. A liquid biopsy capable of capturing and enriching circulating tumor cells (CTCs), together with the possibility of drug screening, is a promising solution. Here, we illustrate the development of a highly efficient ex vivo CTC expansion system based on binary colloidal crystals substrate. Clinical samples were enrolled from 22 patients with SCLC in the study. The CTCs were enriched and expanded from the collected peripheral blood samples. Expanded cells were analyzed for protein expression and observed for drug sensitivity with the use of immunofluorescence and ATP titer evaluation, respectively. Successful CTC spheroid proliferation was established after 4 weeks within 82% of all the collected peripheral blood samples from enrolled patients. Upon immunofluorescence analysis, the enriched cells showed positive markers for EpCAM, TTF-1, synaptophysin and negative for CD45. Additionally, the expanded CTCs demonstrated marked heterogeneity in the expression of E-cadherin and N-cadherin. In a preliminary case series, the drug sensitivity of patient-derived CTC to cisplatin and etoposide was studied to see the correlation with the corresponding therapeutic outcome. In conclusion, our study demonstrates that it is possible to efficiently expand CTCs from SCLC within a clinically relevant time frame; the biomarker information generated from enriched CTCs can assist the selection of effective drugs and improve disease outcome. [ABSTRACT FROM AUTHOR]

Published

2020

16. A Combined Systemic Strategy for Overcoming Cisplatin Resistance in Head and Neck Cancer: From Target Identification to Drug Discovery.

Author

Chen, Yin-Ju, You, Guo-Rung, Lai, Meng-Yu, Lu, Long-Sheng, Chen, Chang-Yu, Ting, Lai-Lei, Lee, Hsin-Lun, Kanno, Yuzuka, Chiou, Jeng-Fong, and Cheng, Ann-Joy

Subjects

CELL lines, CISPLATIN, DRUG resistance, DRUG resistance in cancer cells, DRUG design, HEAD tumors, HYDROCARBONS, NECK tumors, POLYMERASE chain reaction, TERPENES, PHENOTYPES, CELL survival, GENE expression profiling, KAPLAN-Meier estimator

Abstract

Simple Summary: The efficiency of cisplatin is limited by drug resistance in head–neck cancer (HNC) patients. In this study, we established a cisplatin resistance (CR) cell model, generated CR related transcriptome profiling, and combined application of bioinformatics methodology to discover a possible way to overcome CR. Analysis of the functional pathway revealed that mitotic division is a novel mechanism significantly contributing to CR. Spindle pole body component 25 (SPC25), a kinetochore protein, was overexpressed in CR cells and significantly correlated with worse HNC patient survival. The silencing of SPC25 increased cisplatin sensitivity and reduced cancer stemness property. Integration of CR transcriptome profiling and drug database discovered a natural extract compound, celastrol, possessing a potent cytotoxic effect in CR cells to reverse CR. Thus, we combined systemic strategies to demonstrated that a novel biological process (mitotic cell division), a hub gene (SPC25), and a natural compound (celastrol) as novel strategies for the treatment of refractory HNC. Cisplatin is the first-line chemotherapy agent for head and neck cancer (HNC), but its therapeutic effects are hampered by its resistance. In this study, we employed systemic strategies to overcome cisplatin resistance (CR) in HNC. CR cells derived from isogenic HNC cell lines were generated. The CR related hub genes, functional mechanisms, and the sensitizing candidates were globally investigated by transcriptomic and bioinformatic analyses. Clinically, the prognostic significance was assessed by the Kaplan–Meier method. Cellular and molecular techniques, including cell viability assay, tumorsphere formation assay, RT-qPCR, and immunoblot, were used. Results showed that these CR cells possessed highly invasive and stem-like properties. A total of 647 molecules was identified, and the mitotic division exhibited a novel functional mechanism significantly related to CR. A panel of signature molecules, MSRB3, RHEB, ULBP1, and spindle pole body component 25 (SPC25), was found to correlate with poor prognosis in HNC patients. SPC25 was further shown as a prominent molecule, which markedly suppressed cancer stemness and attenuated CR after silencing. Celastrol, a nature extract compound, was demonstrated to effectively inhibit SPC25 expression and reverse CR phenotype. In conclusion, the development of SPC25 inhibitors, such as the application of celastrol, maybe a novel strategy to sensitize cisplatin for the treatment of refractory HNC. [ABSTRACT FROM AUTHOR]

Published

2020

17. Physical Cues in the Microenvironment Regulate Stemness-Dependent Homing of Breast Cancer Cells.

Author

Chu, Hsueh-Yao, Chen, Yin-Ju, Hsu, Chun-Jieh, Liu, Yang-Wei, Chiou, Jeng-Fong, Lu, Long-Sheng, and Tseng, Fan-Gang

Subjects

ALGINATES, BREAST tumors, CELL culture, CELL lines, METASTASIS, PERMEABILITY, DESCRIPTIVE statistics, IN vitro studies

Abstract

Tissue-specific microenvironmental factors contribute to the targeting preferences of metastatic cancers. However, the physical attributes of the premetastatic microenvironment are not yet fully characterized. In this research, we develop a transwell-based alginate hydrogel (TAH) model to study how permeability, stiffness, and roughness of a hanging alginate hydrogel regulate breast cancer cell homing. In this model, a layer of physically characterized alginate hydrogel is formed at the bottom of a transwell insert, which is placed into a matching culture well with an adherent monolayer of breast cancer cells. We found that breast cancer cells dissociate from the monolayer and home to the TAH for continual growth. The process is facilitated by the presence of rich serum in the upper chamber, the increased stiffness of the gel, as well as its surface roughness. This model is able to support the homing ability of MCF-7 and MDA-MB-231 cells drifting across the vertical distance in the culture medium. Cells homing to the TAH display stemness phenotype morphologically and biochemically. Taken together, these findings suggest that permeability, stiffness, and roughness are important physical factors to regulate breast cancer homing to a premetastatic microenvironment. [ABSTRACT FROM AUTHOR]

Published

2020