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Dive into the research topics where Hung-Man Yu is active.

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Featured researches published by Hung-Man Yu.


Molecular Pharmaceutics | 2018

Use of 111In-Hexavalent Lactoside for Liver Reserve Estimation in Rodents with Thioacetamide-Induced Hepatic Fibrosis

Mei-Hui Wang; Chuan-Yi Chien; Hung-Man Yu; Ping-Yen Wang; Wuu-Jyh Lin

Many biochemical tests detecting the presence of liver disease are not liver-specific and may be abnormal in nonhepatic conditions. The asialoglycoprotein receptor (ASGPR) is a hepatocyte-specific receptor for Gal/GalNAc-terminated glycopeptide or glycoprotein. The number of these receptors decreases in patients with chronic liver diseases. Here, we aimed to evaluate the use of 111In-hexavalent lactoside, a known ASGPR imaging biomarker, as a more sensitive probe to detect small changes in liver reserve in animal models of chronic liver injury. Thioacetamide (TAA) treatment via intraperitoneal injection every 2 days in BALB/c mice continued for 1, 2, 3, or 4 months. The liver fibrosis stages were determined by Sirius Red staining and were based on the METAVIR classification method. Serum transaminase enzymes (alanine transaminase (ALT) and aspartate transaminase (AST)), alkaline phosphatase, albumin, and bilirubin were measured using a FUJI FDC3500 i/s analyzer. The ASGPR staining was performed by immunohistocytochemical stain. The percentages of fibrosis and ASGPR were calculated using ImageJ software after collagen staining and anti-ASGPR staining, respectively. A nanoSPECT/CT was used for molecular imaging and liver uptake measurement. We observed fibrosis grades of F0-F1 in mice treated with TAA for 1 month, F2 in mice treated for 2 months, F3-F4 in mice treated for 3 months, and F4 in mice treated for 4 months. The levels of ALT and albumin were not significantly different in the TAA groups from those in the controls. Although the average levels of AST, alkaline phosphatase, and bilirubin in the TAA groups were different from those in the control group, there was little difference between TAA groups. More sensitive distinctions among TAA groups were detected in 111In-hexavalent lactoside uptake of ASGPR, ASGPR staining, and fibrosis % than when using the conventional AST, ALT, albumin, alkaline phosphatase, and bilirubin tests. The absorption and distribution of 111In-hexavalent lactoside were lower in the chronic hepatitis models than the normal controls. The liver reserves measured by 111In-hexavalent lactoside uptake were 71.7 ± 7.5% and 50.9 ± 5.6% after 1 and 2 months, respectively, of TAA treatment. As an ASGPR biomarker, 111In-hexavalent lactoside has higher sensitivity than traditional liver function tests and collagen stain to provide more objective data for evaluating compensated cirrhosis or changes in liver damage. ASGPR staining can reflect the regenerated hepatocytes, but the need for a biopsy limits its use. 111In-hexavalent lactoside measurement is comparable with ASGPR staining, which suggests that 111In-hexavalent lactoside measurement will be more useful as a practical, noninvasive test of chronic liver injury.


The Journal of Nuclear Medicine | 2004

Antisense Thymidylate Synthase Electrogene Transfer to Increase Uptake of Radiolabeled Iododeoxyuridine in a Murine Model

Kwan-Hwa Chi; Hsin-Ell Wang; Yu-Shan Wang; Shun-Lan Chou; Hung-Man Yu; Yu-Hua Tseng; Ing-Ming Hwang; Wing-Yiu Lui


Biochemical Pharmacology | 2005

Modulation of 5-fluorouracil cytotoxicity through thymidylate synthase and NF-κB down-regulation and its application on the radiolabelled iododeoxyuridine therapy on human hepatoma cell

Hsin-Ell Wang; Hui-Chuan Wu; Shang-Jyh Kao; Fan-Wei Tseng; Yu-Shan Wang; Hung-Man Yu; Shun-Lan Chou; Sang-Hue Yen; Kwan-Hwa Chi


Journal of Labelled Compounds and Radiopharmaceuticals | 2018

Development of single vial kits for preparation of 68Ga-labelled hexavalent lactoside for PET imaging of asialoglycoprotein receptor

Hung-Man Yu; Chen-Hsin Chan; Jyun-Hong Chen; Chuan-Yi Chien; Ping-Yen Wang; Wei-Cheng Juan; Chun-Hung Yang; Hao-Ting Hsia; Mei-Hui Wang; Wuu-Jyh Lin


The Journal of Nuclear Medicine | 2011

Pre-clinical research in developing a molecular imaging probe for non-invasive early detection of human ovarian cancers

Mao-Chi Weng; Hung-Man Yu; Mei-Hui Wang; Wei-Ti Kuo; Jia-Wei Kuo; Chuan-Yi Chien; Ping-Yen Wang; Wuu-Jyh Lin


Society of Nuclear Medicine Annual Meeting Abstracts | 2011

Potential evaluation of 111In-Hexa lactoside as a novel functional liver imaging agent

Ping-Yen Wang; Chuan-Yi Chien; Hung-Man Yu; Mei-Hui Wang; Mao-Chi Weng; Wei-Ti Kuo; Jia-Wei Kuo; Wuu-Jyh Lin


Society of Nuclear Medicine Annual Meeting Abstracts | 2011

Toxicity and safety evaluation of multivalent lactoside for asialoglycoprotein receptor imaging

Hung-Man Yu; Mei-Hui Wang; Chuan-Yi Chien; Ping-Yen Wang; Mao-Chi Weng; Wei-Ti Kuo; Ying-Xun Chang; Jia-Wei Kuo; Jen-Tsung Wang; Wuu-Jyh Lin


Society of Nuclear Medicine Annual Meeting Abstracts | 2011

Biodistribution, pharmacokinetic and radiation dosimetry of 111In-DTPA hexa lactoside

Chuan-Yi Chien; Jia-Wei Kuo; Mao-Chi Weng; Hung-Man Yu; Mei-Hui Wang; Ping-Yen Wang; Wei-Ti Kuo; Wuu-Jyh Lin


Archive | 2011

RADIOLABELED NUCLEOSIDE ANALOGUE, AND PREPARATION METHOD AND USE THEREOF

Hsin-Ell Wang; Chih-Yuan Lin; Wei-Ti Kuo; Chuan-Lin Chen; Mei-Hui Wang; Hung-Man Yu; Mao-Chi Weng; Yu Chang; Wuu-jyh Lin


Society of Nuclear Medicine Annual Meeting Abstracts | 2007

A novel imaging proprobe for monitoring prodrug-activating enzyme in vivo

Hsin-Ell Wang; Tian-Lu Cheng; Hung-Man Yu; Yu-Cheng Su; Hsin-Pei Yeh; Jia-Je Li

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Mei-Hui Wang

National Yang-Ming University

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Hsin-Ell Wang

National Yang-Ming University

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Mao-Chi Weng

National Yang-Ming University

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Wei-Ti Kuo

National Yang-Ming University

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Kwan-Hwa Chi

Memorial Hospital of South Bend

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Hsin-Pei Yeh

National Yang-Ming University

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Shun-Lan Chou

National Yang-Ming University

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