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Dive into the research topics where Amin Soebandrio is active.

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Featured researches published by Amin Soebandrio.


Shock | 2014

ABANDON THE MOUSE RESEARCH SHIP? NOT JUST YET!

Marcin F. Osuchowski; Daniel G. Remick; James A. Lederer; Charles H. Lang; Ansgar O. Aasen; Mayuki Aibiki; Luciano C. P. Azevedo; Soheyl Bahrami; Mihály Boros; Robert N. Cooney; Salvatore Cuzzocrea; Yong Jiang; Wolfgang G. Junger; Hiroyuki Hirasawa; Richard S. Hotchkiss; Xiang-An Li; Peter Radermacher; Heinz Redl; Reinaldo Salomão; Amin Soebandrio; Christoph Thiemermann; Jean Louis Vincent; Peter A. Ward; Yong Ming Yao; Huang Ping Yu; Basilia Zingarelli; Irshad H. Chaudry

ABSTRACT Many preclinical studies in critical care medicine and related disciplines rely on hypothesis-driven research in mice. The underlying premise posits that mice sufficiently emulate numerous pathophysiologic alterations produced by trauma/sepsis and can serve as an experimental platform for answering clinically relevant questions. Recently, the lay press severely criticized the translational relevance of mouse models in critical care medicine. A series of provocative editorials were elicited by a highly publicized research report in the Proceedings of the National Academy of Sciences (PNAS; February 2013), which identified an unrecognized gene expression profile mismatch between human and murine leukocytes following burn/trauma/endotoxemia. Based on their data, the authors concluded that mouse models of trauma/inflammation are unsuitable for studying corresponding human conditions. We believe this conclusion was not justified. In conjunction with resulting negative commentary in the popular press, it can seriously jeopardize future basic research in critical care medicine. We will address some limitations of that PNAS report to provide a framework for discussing its conclusions and attempt to present a balanced summary of strengths/weaknesses of use of mouse models. While many investigators agree that animal research is a central component for improved patient outcomes, it is important to acknowledge known limitations in clinical translation from mouse to man. The scientific community is responsible to discuss valid limitations without overinterpretation. Hopefully, a balanced view of the strengths/weaknesses of using animals for trauma/endotoxemia/critical care research will not result in hasty discount of the clear need for using animals to advance treatment of critically ill patients.


Japanese Journal of Infectious Diseases | 2016

Anti-hepatitis C virus activity of a crude extract from longan ( Dimocarpus longan Lour.) leaves

Dadan Ramadhan Apriyanto; Chie Aoki; Sri Hartati; Muhammad Hanafi; Leonardus B S Kardono; Ade Arsianti; Melva Louisa; Tjahjani M. Sudiro; Beti Ernawati Dewi; Pratiwi Sudarmono; Amin Soebandrio; Hak Hotta

Infection with hepatitis C virus (HCV) results in hepatitis C, a disease characterized by chronic infection, cirrhosis, and hepatocellular carcinoma. Currently, the standard therapy is a combination of pegylated interferon-α plus ribavirin with NS3 protease inhibitors. Addition of NS3 protease inhibitors to the standard therapy improves response rates; however, use of NS3 protease inhibitors is also associated with significant adverse effects and an increase in the overall cost of treatment. Therefore, there is a need to develop safe and inexpensive drugs for the treatment of HCV infections. In this study, we examined the antiviral activity of a crude extract from Dimocarpus longan leaves against HCV (genotype 2a strain JFH1). The D. longan crude extract (DL-CE) exhibited anti-HCV activity with a 50% effective concentration (EC50) of 19.4 μg/ml without cytotoxicity. A time-of-addition study demonstrated that DL-CE has anti-HCV activity at both the entry and post-entry steps and markedly blocks the viral entry step through direct virucidal activity with marginal inhibition of virion assembly. Co-treatment of DL-CE with cyclosporine A, an immunosuppressant or telaprevir, an NS3 protease inhibitor, resulted in additive and synergistic antiviral effects, respectively. Our findings suggest that DL-CE may be useful as an add-on therapy candidate for treating HCV infections.


Tropical Doctor | 2018

Laboratory parameters for predicting Salmonella bacteraemia: a prospective cohort study

Suhendro Suwarto; Hadianti Adlani; Leonard Nainggolan; Cleopas Martin Rumende; Amin Soebandrio

Blood cultures for a definitive diagnosis of typhoid fever takes time and are not routinely available. We thus investigated laboratory parameters to predict Salmonella bacteraemia. We conducted a prospective cohort study in Jakarta, Indonesia. Patients with suspected typhoid fever admitted to hospital from October 2014 to December 2016 were included. Out of 187 individuals, 27 had Salmonella typhi and 12 had S. paratyphi in blood cultures. Absolute eosinopenia, elevated aspartate aminotransferase and elevated C-reactive protein > 40 mg/L were positive predictors.


Virology | 2013

Antigenic Variation in H5N1 clade 2.1 Viruses in Indonesia From 2005 to 2011

Vivi Setiawaty; Eka Pratiwi; Hana A. Pawestri; Fera Ibrahim; Amin Soebandrio

Influenza A (H5N1) virus, has spread to several countries in the world and has a high mortality rate. Meanwhile, the virus has evolved into several clades. The human influenza A (H5N1) virus circulating in Indonesia is a member of clade 2.1, which is different in antigenicity from other clades of influenza A (H5N1). An analysis of the antigenic variation in the H5 hemagglutinin gene (HA) of the influenza A (H5N1) virus strains circulating in Indonesia has been undertaken. Several position of amino acid mutations, including mutations at positions 35, 53, 141, 145, 163, 174, 183, 184, 189, and 231, have been identified. The mutation Val-174-Iso appears to play an important role in immunogenicity and cross-reactivity with rabbit antisera. This study shows that the evolution of the H5HA antigenic variation of the influenza A (H5N1) virus circulating in Indonesia from 2005 to 2011 may affect the immunogenicity of the virus.


Journal of Biochemistry | 1985

Native and non-native conformation-specific antibodies directed to the loop region of hen egg-white lysozyme.

Hajime Fujio; Yutaka Takagaki; Youn-Mun Ha; Elvira Missako Doi; Amin Soebandrio; Nobuo Sakato


Microbiology Indonesia | 2011

The Genetic Drift of Indonesian Avian Influenza A H5N1 Viruses During 2003-2008

Ni Luh Putu Indi Dharmayanti; Gina Samaan; Fera Ibrahim; Risa Indriani; Darminto; Amin Soebandrio


Hayati Journal of Biosciences | 2011

Influenza H5N1 Virus of Birds Surrounding H5N1 Human Cases Have Specific Characteristics on the Matrix Protein

Ni Luh Putu Indi Dharmayanti; Fera Ibrahim; Darminto; Amin Soebandrio


Medical Journal of Indonesia | 2000

Resistance pattern of Mycobacterium tuberculosis to first-line antituberculosis drugs

Tjahjani M. Sudiro; Amin Soebandrio; Prawoto Prawoto; Pratiwi Sudarmono


Journal of Biochemistry | 1987

Specificity Change of Antibody to (4-Hydroxy-3-Nitrophenyl)Acetyl Haptens by Somatic Hypermutation

Amin Soebandrio; Takachika Azuma; Yoshio Hamada; Nobuo Sakato; Hajime Fujio


Archive | 2014

Review Article ABANDON THE MOUSE RESEARCH SHIP? NOT JUST YET!

Marcin F. Osuchowski; Daniel G. Remick; James A. Lederer; Charles H. Lang; Ansgar O. Aasen; Mayuki Aibiki; Luciano C. P. Azevedo; Soheyl Bahrami; Mihály Boros; Robert N. Cooney; Salvatore Cuzzocrea; Yong Jiang; Wolfgang G. Junger; Hiroyuki Hirasawa; Richard S. Hotchkiss; Xiang-An Li; Peter Radermacher; Heinz Redl; Reinaldo Salomão; Amin Soebandrio; Christoph Thiemermann; Jean Louis Vincent; Peter A. Ward; Y. M. Yao; Huang-Ping Yu; Basilia Zingarelli; Irshad H. Chaudry

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Fera Ibrahim

University of Indonesia

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Basilia Zingarelli

Cincinnati Children's Hospital Medical Center

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Charles H. Lang

Penn State Milton S. Hershey Medical Center

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Irshad H. Chaudry

University of Alabama at Birmingham

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