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Hyun Park	9 Articles
Evaluation of the antimalarial activity of SAM13-2HCl with morpholine amide (SKM13 derivative) against antimalarial drug-resistant Plasmodium falciparum and Plasmodium berghei infected ICR mice Hyelee Hong, Kwonmo Moon, Thuy-Tien Thi Trinh, Tae-Hui Eom, Hyun Park, Hak Sung Kim, Seon-Ju Yeo Parasites Hosts Dis 2024;62(1):42-52. Published online February 23, 2024 DOI: https://doi.org/10.3347/PHD.23093 Abstract PDF Supplementary Material Antimalarial drugs are an urgently need and crucial tool in the campaign against malaria, which can threaten public health. In this study, we examined the cytotoxicity of the 9 antimalarial compounds chemically synthesized using SKM13-2HCl. Except for SKM13-2HCl, the 5 newly synthesized compounds had a 50% cytotoxic concentration (CC₅₀) > 100 µM, indicating that they would be less cytotoxic than SKM13-2HCl. Among the 5 compounds, only SAM13-2HCl outperformed SKM13-2HCl for antimalarial activity, showing a 3- and 1.3-fold greater selective index (SI) (CC₅₀/IC₅₀) than SKM13-2HCl in vitro against both chloroquine-sensitive (3D7) and chloroquine -resistant (K1) Plasmodium falciparum strains, respectively. Thus, the presence of morpholine amide may help to effectively suppress human-infectious P. falciparum parasites. However, the antimalarial activity of SAM13-2HCl was inferior to that of the SKM13-2HCl template compound in the P. berghei NK65-infected mouse model, possibly because SAM13-2HCl had a lower polarity and less efficient pharmacokinetics than SKM13-2HCl. SAM13-2HCl was more toxic in the rodent model. Consequently, SAM13-2HCl containing morpholine was selected from screening a combination of pharmacologically significant structures as being the most effective in vitro against human-infectious P. falciparum but was less efficient in vivo in a P. berghei-infected animal model when compared with SKM13-2HCl. Therefore, SAM13-2HCl containing morpholine could be considered a promising compound to treat chloroquine-resistant P. falciparum infections, although further optimization is crucial to maintain antimalarial activity while reducing toxicity in animals. Citations Citations to this article as recorded by The Importance of Murine Models in Determining In Vivo Pharmacokinetics, Safety, and Efficacy in Antimalarial Drug Discovery Glory Adebayo, Opeyemi I. Ayanda, Matthias Rottmann, Olusola S. Ajibaye, Gbolahan Oduselu, Julius Mulindwa, Olayinka O. Ajani, Oluwagbemiga Aina, Pascal Mäser, Ezekiel Adebiyi Pharmaceuticals.2025; 18(3): 424. CrossRef Structural, electrochemical and theoretical studies of some carboxamides David Izuchukwu Ugwu, Nandisiwe GS Mateyise, Jeanet Conradie Journal of Molecular Structure.2025; 1348: 143454. CrossRef 5,569 View 119 Download 2 Web of Science Crossref In Vitro Evaluation of Two Novel Antimalarial Derivatives of SKM13: SKM13-MeO and SKM13-F Thuy-Tien Thi Trinh, Young-ah Kim, Hyelee Hong, Linh Thi Thuy Le, Hayoung Jang, Soon-Ai Kim, Hyun Park, Hak Sung Kim, Seon-Ju Yeo Korean J Parasitol 2022;60(6):401-407. Published online December 22, 2022 DOI: https://doi.org/10.3347/kjp.2022.60.6.401 Abstract PDF Supplementary Material Antimalarial drugs play an important role in the control and treatment of malaria, a deadly disease caused by the protozoan parasite Plasmodium spp. The development of novel antimalarial agents effective against drug-resistant malarial parasites is urgently needed. The novel derivatives, SKM13-MeO and SKM13-F, were designed based on an SKM13 template by replacing the phenyl group with electron-donating (-OMe) or electron-withdrawing groups (-F), respectively, to reverse the electron density. A colorimetric assay was used to quantify cytotoxicity, and in vitro inhibition assays were performed on 3 different blood stages (ring, trophozoite, and schizonts) of P. falciparum 3D7 and the ring/mixed stage of D6 strain after synchronization. The in vitro cytotoxicity analysis showed that 2 new SKM13 derivatives reduced the cytotoxicity of the SKM13 template. SKM13 maintained the IC₅₀ at the ring and trophozoite stages but not at the schizont stage. The IC₅₀ values for both the trophozoite stage of P. falciparum 3D7 and ring/mixed stages of D6 demonstrated that 2 SKM13 derivatives had decreased antimalarial efficacy, particularly for the SKM13-F derivative. SKM13 may be comparably effective in ring and trophozoite, and electron-donating groups (-OMe) may be better maintain the antimalarial activity than electron-withdrawing groups (-F) in SKM13 modification. Citations Citations to this article as recorded by Design, Synthesis and in vitro Evaluation of Primaquine and Diaminoquinazoline Hybrid Molecules Against the Malaria Parasite Mukul Kore, Anjani G. Rao, Dimple Acharya, Shrikant S. Kirwale, Amritansh Bhanot, Abhishek Govekar, Ajeet Kumar Mohanty, Aniruddha Roy, Shruthi S. Vembar, Sandeep Sundriyal Chemistry – An Asian Journal.2025;[Epub] CrossRef Evaluation of the antimalarial activity of SAM13-2HCl with morpholine amide (SKM13 derivative) against antimalarial drug-resistant Plasmodium falciparum and Plasmodium berghei infected ICR mice Hyelee Hong, Kwonmo Moon, Thuy-Tien Thi Trinh, Tae-Hui Eom, Hyun Park, Hak Sung Kim, Seon-Ju Yeo Parasites, Hosts and Diseases.2024; 62(1): 42. CrossRef 3,436 View 141 Download 2 Web of Science Crossref Development of Monoclonal Antibodies for Diagnosis of Plasmodium vivax Nguyen Thi Phuong Linh, Hyun Park, Jinyoung Lee, Dong-Xu Liu, Ga-Eun Seo, Hae-Jin Sohn, Jin-Hee Han, Eun-Taek Han, Ho-Joon Shin, Seon-Ju Yeo Korean J Parasitol 2017;55(6):623-630. Published online December 31, 2017 DOI: https://doi.org/10.3347/kjp.2017.55.6.623 Abstract PDF Plasmodium lactate dehydrogenase (pLDH) is a strong target antigen for the determination of infection with Plasmodium species specifically. However, a more effective antibody is needed because of the low sensitivity of the current antibody in many immunological diagnostic assays. In this study, recombinant Plasmodium vivax LDH (PvLDH) was experimentally constructed and expressed as a native antigen to develop an effective P. vivax-specific monoclonal antibody (mAb). Two mAbs (2CF5 and 1G10) were tested using ELISA and immunofluorescence assays (IFA), as both demonstrated reactivity against pLDH antigen. Of the 2 antibodies, 2CF5 was not able to detect P. falciparum, suggesting that it might possess P. vivax-specificity. The detection limit for a pair of 2 mAbs-linked sandwich ELISA was 31.3 ng/ml of the recombinant antigen. The P. vivax-specific performance of mAbs-linked ELISA was confirmed by in vitro-cultured P. falciparum and P. vivax-infected patient blood samples. In conclusion, the 2 new antibodies possessed the potential to detect P. vivax and will be useful in immunoassay. Citations Citations to this article as recorded by Diagnostic Methods for Non-Falciparum Malaria Alba Marina Gimenez, Rodolfo F. Marques, Matías Regiart, Daniel Youssef Bargieri Frontiers in Cellular and Infection Microbiology.2021;[Epub] CrossRef Plasmodium falciparum Parasitemia and Band Sensitivity of the SD Bioline Malaria Ag P.f/Pan Rapid Diagnostic Test in Madagascar Rajeev K. Mehlotra, Rosalind E. Howes, Estee Y. Cramer, Riley E. Tedrow, Tovonahary A. Rakotomanga, Stéphanie Ramboarina, Arsène C. Ratsimbasoa, Peter A. Zimmerman The American Journal of Tropical Medicine and Hygiene.2019; 100(5): 1196. CrossRef 9,246 View 234 Download 4 Web of Science Crossref Antimalarial Activity of C-10 Substituted Triazolyl Artemisinin Gab-Man Park, Hyun Park, Sangtae Oh, Seokjoon Lee Korean J Parasitol 2017;55(6):661-665. Published online December 31, 2017 DOI: https://doi.org/10.3347/kjp.2017.55.6.661 Abstract PDF We synthesized C-10 substituted triazolyl artemisinins by the Huisgen cycloaddition reaction between dihydroartemisinins (2) and variously substituted 1, 2, 3-triazoles (8a-8h). The antimalarial activities of 32 novel artemisinin derivatives were screened against a chloroquine-resistant parasite. Among them, triazolyl artemisinins with electron-withdrawing groups showed stronger antimalarial activities than those shown by the derivatives having electron-donating groups. In particularly, m-chlorotriazolyl artemisinin (9d-12d) showed antimalarial activity equivalent to that of artemisinin and could be a strong drug candidate. Citations Citations to this article as recorded by Novel frontiers through nitrogen substitution at 6th, 10th and 11th position of artemisinin: Synthetic approaches and antimalarial activity Priyanka Yadav, Varun Rawat, Shalini Kaushik Love, Ved Prakash Verma European Journal of Medicinal Chemistry.2025; 281: 117032. CrossRef Identification of potential bi-triazole based antimalarial compounds and their effects against asexual stages of Plasmodium isolates Marcinete Latorre Almeida, Leandro do Nascimento Martinez, Welington da Silva Paula do Nascimento, Guilherme Matos Passarini, Daniel Sol Sol de Medeiros, Minelly Azevedo da Silva, Saara Neri Fialho, Amália do Santos Ferreira, Norton Rubens Diunior Lucas P Caderno Pedagógico.2024; 21(13): e12709. CrossRef In silico screening, synthesis, and antimalarial evaluation of PABA substituted 1,3,5-triazine derivatives as Pf-DHFR inhibitors Ashmita Saha, Ayesha Aktar Khanam Choudhury, Nayana Adhikari, Surajit Kumar Ghosh, Anshul Shakya, Saurav Jyoti Patgiri, Udaya Pratap Singh, Hans Raj Bhat Experimental Parasitology.2023; 250: 108546. CrossRef Current development of 1,2,3-triazole derived potential antimalarial scaffolds: Structure- activity relationship (SAR) and bioactive compounds S. Maheen Abdul Rahman, Jasvinder Singh Bhatti, Suresh Thareja, Vikramdeep Monga European Journal of Medicinal Chemistry.2023; 259: 115699. CrossRef Exploration of artemisinin derivatives and synthetic peroxides in antimalarial drug discovery research Om P.S. Patel, Richard M. Beteck, Lesetja J. Legoabe European Journal of Medicinal Chemistry.2021; 213: 113193. CrossRef 7,703 View 173 Download 6 Web of Science Crossref In Vitro and in Vivo Effects of Nitrofurantoin on Experimental Toxoplasmosis Seon-Ju Yeo, ChunMei Jin, SungYeon Kim, Hyun Park Korean J Parasitol 2016;54(2):155-161. Published online April 30, 2016 DOI: https://doi.org/10.3347/kjp.2016.54.2.155 Abstract PDF Toxoplasma gondii is an important opportunistic pathogen that causes toxoplasmosis, which has very few therapeutic treatment options. The most effective therapy is a combination of pyrimethamine and sulfadiazine; however, their utility is limited because of drug toxicity and serious side effects. For these reasons, new drugs with lower toxicity are urgently needed. In this study, the compound, (Z)-1-[(5-nitrofuran-2-yl)methyleneamino]-imidazolidine-2,4-dione (nitrofurantoin), showed anti-T. gondii effects in vitro and in vivo. In HeLa cells, the selectivity of nitrofurantoin was 2.3, which was greater than that of pyrimethamine (0.9). In T. gondii-infected female ICR mice, the inhibition rate of T. gondii growth in the peritoneal cavity was 44.7% compared to the negative control group after 4-day treatment with 100 mg/kg of nitrofurantoin. In addition, hematology indicators showed that T. gondii infection-induced serum alanine aminotransferase (ALT) and aspartate aminotransferase (AST) levels, biochemical parameters involved in liver injury, were reduced by nitrofurantoin significantly. Moreover, nitrofurantoin exerted significant effects on the index of antioxidant status, i.e., malondialdehyde (MDA) and glutathione (GSH). The nitrofurantoin-treated group inhibited the T. gondii-induced MDA levels while alleviating the decrease in GSH levels. Thus, nitrofurantoin is a potential anti-T. gondii candidate for clinical application. Citations Citations to this article as recorded by Avian trichomonosis: An innovative approach in drug redirection with Ciprofloxacin, Norfloxacin, and Nitrofurantoin Marjorie de Giacometi, Yan Wahast Islabão, Alexia Brauner de Mello, Filipe Obelar Martins, Melinda Gomes Victor, Camila Belmonte Oliveira Parasitology International.2026; 112: 103221. CrossRef Extracts of food and medicinal plants sold in Moroccan markets induce apoptosis-like in Toxoplasma gondii tachyzoites in vitro Ismail Elkoraichi, Nathalie Moiré, Samira Rais, Isabelle Dimier-Poisson, Fouad Daoudi, Françoise Debierre-Grockiego Scientific African.2025; 27: e02529. CrossRef Efficacy of nitrofurantoin in treatment of murine model of trichinellosis Basma M. Elmansory, Hager S. Zoghroban, Dina M. El-Guindy, Dina A. El-Guindy Experimental Parasitology.2025; 277: 109022. CrossRef The Brazilian Toxoplasma gondii strain BRI caused greater inflammation and impairment in anxiogenic behavior in mice, which was reverted by rosuvastatin treatment Fernanda Ferreira Evangelista, Priscilla de Laet Sant’Ana, Willian Costa Ferreira, Thaisa Andreia Ferreira, Milena Lopes dos Santos, Amanda Hinobu de Souza, Felipe Aparecido Lacerda de Andrade, Douglas Aparecido da Silva, Luiz Daniel de Barros, Cristiane Parasitology Research.2024;[Epub] CrossRef Inclusion of Nitrofurantoin into the Realm of Cancer Chemotherapy via Biology-Oriented Synthesis and Drug Repurposing Perihan A. Elzahhar, Hisham A. Nematalla, Houssam Al-Koussa, Carla Abrahamian, Amira F. El-Yazbi, Larry Bodgi, Jolie Bou-Gharios, Joyce Azzi, Joelle Al Choboq, Hala F. Labib, Wassim Abou Kheir, Marwa M. Abu-Serie, Mohamed A. Elrewiny, Ahmed F. El-Yazbi, A Journal of Medicinal Chemistry.2023; 66(7): 4565. CrossRef Evaluation of mono and combined nitrofurantoin therapy for toxoplasmosis in vivo using murine model Asmaa Elkholy, Rita Wassef, Omnia Alsaid, Mona Elawady, Ashraf Barakat, Ashraf Soror, Shereen Kishik Pathogens and Global Health.2023; 117(7): 664. CrossRef Old Dogs with New Tricks: Antiparasitic Potential of Structurally Diverse 5-Nitrofuran and 5-Nitrothiophene Imines and Acyl Hydrazones Ibrahim S. Al Nasr, Waleed S. Koko, Tariq A. Khan, Rainer Schobert, Bernhard Biersack Scientia Pharmaceutica.2023; 91(3): 44. CrossRef Anti-Toxoplasma gondii agent isolated from Orostachys malacophylla (Pallas) Fischer Yan Piao, Lili Jin, Xu Cheng, Weifeng Yan, Changhao Zhang, Sihong Wang, Chunmei Jin Experimental Parasitology.2022; 242: 108397. CrossRef Recent Advances in the Synthesis and Development of Nitroaromatics as Anti-Infective Drugs Christina Kannigadu, David. D. N'Da Current Pharmaceutical Design.2020; 26(36): 4658. CrossRef Safety and efficacy of the bumped kinase inhibitor BKI-1553 in pregnant sheep experimentally infected with Neospora caninum tachyzoites Roberto Sánchez-Sánchez, Ignacio Ferre, Michela Re, Patricia Vázquez, Luis Miguel Ferrer, Javier Blanco-Murcia, Javier Regidor-Cerrillo, Manuel Pizarro Díaz, Marta González-Huecas, Enrique Tabanera, Paula García-Lunar, Julio Benavides, Pablo Castaño, Andr International Journal for Parasitology: Drugs and Drug Resistance.2018; 8(1): 112. CrossRef A Systematic Review of In vitro and In vivo Activities of Anti-Toxoplasma Drugs and Compounds (2006–2016) Mahbobeh Montazeri, Mehdi Sharif, Shahabeddin Sarvi, Saeed Mehrzadi, Ehsan Ahmadpour, Ahmad Daryani Frontiers in Microbiology.2017;[Epub] CrossRef Lectins from Synadenium carinatum (ScLL) and Artocarpus heterophyllus (ArtinM) Are Able to Induce Beneficial Immunomodulatory Effects in a Murine Model for Treatment of Toxoplasma gondii Infection Eliézer L. P. Ramos, Silas S. Santana, Murilo V. Silva, Fernanda M. Santiago, Tiago W. P. Mineo, José R. Mineo Frontiers in Cellular and Infection Microbiology.2016;[Epub] CrossRef 10,348 View 129 Download 13 Web of Science Crossref Potential Interaction of Plasmodium falciparum Hsp60 and Calpain Seon-Ju Yeo, Dong-Xu Liu, Hyun Park Korean J Parasitol 2015;53(6):665-673. Published online December 31, 2015 DOI: https://doi.org/10.3347/kjp.2015.53.6.665 Abstract PDF After invasion of red blood cells, malaria matures within the cell by degrading hemoglobin avidly. For enormous protein breakdown in trophozoite stage, many efficient and ordered proteolysis networks have been postulated and exploited. In this study, a potential interaction of a 60-kDa Plasmodium falciparum (Pf)-heat shock protein (Hsp60) and Pf-calpain, a cysteine protease, was explored. Pf-infected RBC was isolated and the endogenous Pf-Hsp60 and Pf-calpain were determined by western blot analysis and similar antigenicity of GroEL and Pf-Hsp60 was determined with anti-Pf-Hsp60. Potential interaction of Pf-calpain and Pf-Hsp60 was determined by immunoprecipitation and immunofluorescence assay. Mizoribine, a well-known inhibitor of Hsp60, attenuated both Pf-calpain enzyme activity as well as P. falciparum growth. The presented data suggest that the Pf-Hsp60 may function on Pf-calpain in a part of networks during malaria growth. Citations Citations to this article as recorded by To explore molecular targets and combination antimalarial chemotherapeutics as tissue and erythrocytic schizonticides Shilpa Mandal, Nehadrita Chattoraj, Sisir Nandi, Asmita Samadder Journal of Parasitic Diseases.2025;[Epub] CrossRef Controlling drug resistance by targeting Plasmodium falciparum heat shock protein 70-1, a chaperone at the centre of protein quality control mechanism: a review Douglas A. M. Ruhwaya, Brilliant Nyathi, Gadzikano Munyuki, Ryman Shoko, Grace Mugumbate All Life.2023;[Epub] CrossRef Development of a Rapid Fluorescent Diagnostic System to Detect Subtype H9 Influenza A Virus in Chicken Feces Hien Thi Tuong, Ju Hwan Jeong, Young Ki Choi, Hyun Park, Yun Hee Baek, Seon-Ju Yeo International Journal of Molecular Sciences.2021; 22(16): 8823. CrossRef Small Molecule Inhibitors Targeting the Heat Shock Protein System of Human Obligate Protozoan Parasites Tawanda Zininga, Addmore Shonhai International Journal of Molecular Sciences.2019; 20(23): 5930. CrossRef Development of a Rapid Fluorescent Immunochromatographic Test to Detect Respiratory Syncytial Virus Trinh Thi Thuy Tien, Hyun Park, Hien Thi Tuong, Seung-Taek Yu, Du-Young Choi, Seon-Ju Yeo International Journal of Molecular Sciences.2018; 19(10): 3013. CrossRef Rapid detection of avian influenza A virus by immunochromatographic test using a novel fluorescent dye Seon-Ju Yeo, Bui Thi Cuc, Soon-Ai Kim, Do Thi Hoang Kim, Duong Tuan Bao, Trinh Thi Thuy Tien, Nguyen Thi Viet Anh, Do-Young Choi, Chom-Kyu Chong, Hak Sung Kim, Hyun Park Biosensors and Bioelectronics.2017; 94: 677. CrossRef Improvement of a rapid diagnostic application of monoclonal antibodies against avian influenza H7 subtype virus using Europium nanoparticles Seon-Ju Yeo, Duong Tuan Bao, Ga-Eun Seo, Cuc Thi Bui, Do Thi Hoang Kim, Nguyen Thi Viet Anh, Trinh Thi Thuy Tien, Nguyen Thi Phuong Linh, Hae-Jin Sohn, Chom-Kyu Chong, Ho-Joon Shin, Hyun Park Scientific Reports.2017;[Epub] CrossRef 10,710 View 110 Download 8 Web of Science Crossref Expression of Exogenous Human Hepatic Nuclear Factor-1α by a Lentiviral Vector and Its Interactions with Plasmodium falciparum Subtilisin-Like Protease 2 Shunyao Liao, Yunqiang Liu, Bing Zheng, Pyo Yun Cho, Hyun Ok Song, Yun-Seok Lee, Suk-Yul Jung, Hyun Park Korean J Parasitol 2011;49(4):431-436. Published online December 16, 2011 DOI: https://doi.org/10.3347/kjp.2011.49.4.431 Abstract PDF The onset, severity, and ultimate outcome of malaria infection are influenced by parasite-expressed virulence factors as well as by individual host responses to these determinants. In both humans and mice, liver injury follows parasite entry, persisting to the erythrocytic stage in the case of infection with the fatal strain of Plasmodium falciparum. Hepatic nuclear factor (HNF)-1α is a master regulator of not only the liver damage and adaptive responses but also diverse metabolic functions. In this study, we analyzed the expression of host HNF-1α in relation to malaria infection and evaluated its interaction with the 5'-untranslated region of subtilisin-like protease 2 (subtilase, Sub2). Recombinant human HNF-1α expressed by a lentiviral vector (LV HNF-1α) was introduced into mice. Interestingly, differences in the activity of the 5'-untranslated region of the Pf-Sub2 promoter were detected in 293T cells, and LV HNF-1α was observed to influence promoter activity, suggesting that host HNF-1α interacts with the Sub2 gene. 8,716 View 67 Download Transcriptional Activity of Plasmodium Subtilisin-like Protease 2 (Pf-Sub2) 5'Untranslated Regions and Its Interaction with Hepatocyte Growth Factor Shunyao Liao, Yunqiang Liu, Suk-Yul Jung, Pyo Yun Cho, Bing Zheng, Hyun Park Korean J Parasitol 2010;48(4):291-295. Published online December 16, 2010 DOI: https://doi.org/10.3347/kjp.2010.48.4.291 Abstract PDF The onset, severity, and ultimate outcome of malaria infection are influenced by parasite-expressed virulence factors and individual host responses to these determinants. In both humans and mice, liver injury is involved after parasite entry, which persists until the erythrocyte stage after infection with the fatal strain Plasmodium falciparum (Pf). Hepatocyte growth factor (HGF) has strong anti-apoptotic effects in various kinds of cells, and also has diverse metabolic functions. In this work, Pf-subtilisin-like protease 2 (Pf-Sub2) 5'untranslated region (UTR) was analyzed and its transcriptional activity was estimated by luciferase expression. Fourteen TATA boxes were observed but only one Oct-1 and c-Myb were done. In addition, host HGF interaction with Pf-Sub2 was evaluated by co-transfection of HGF- and Pf-Sub2-cloned vector. Interestingly, -1,422/+12 UTR exhibited the strongest luciferase activity but -329 to +12 UTR did not exhibit luciferase activity. Moreover, as compared with the control of unexpressed HGF, the HGF protein suppressed luciferase expression driven by the 5'untranslated region of the Pf-Sub2 promoter. Taken together, it is suggested that HGF controls and interacts with the promoter region of the Pf-Sub2 gene. Citations Citations to this article as recorded by Characterization of the transcriptome and temperature-induced differential gene expression in QPX, the thraustochytrid parasite of hard clams Ewelina Rubin, Arnaud Tanguy, Mickael Perrigault, Emmanuelle Pales Espinosa, Bassem Allam BMC Genomics.2014;[Epub] CrossRef 9,104 View 78 Download Crossref Biological and biochemical modulation of Trichomonas vaginalis KT9 isolate after shifting of culture medium from TPS-1 into TYM Jae-Sook Ryu, Ryung Choi, So-Young Park, Hyun Park, Duk-Young Min Korean J Parasitol 1998;36(4):255-260. Published online December 20, 1998 DOI: https://doi.org/10.3347/kjp.1998.36.4.255 Abstract PDF To evaluate the biological and biochemical characteristics of Trichomonas vaginalis KT9 isolate, the growth and size of trichomonads, pathogenicity in mouse, protein profiles and proteinase activity were examined after shifting the medium from TPS-1 into TYM. Generation time of trichomonads in TYM medium was 4.5 hr in comparison to TPS-1 with 7.1 hr. Size of trichomonads cultured in TPS-1 medium (8.5 ± 0.9 × 6.0 ± 0.9 ?m) was significantly smaller than those in TYM medium (10.9 ± 1.4 × 8.2 ± 0.9 ?m). Trichomonads cultured in TYM medium produced subcutaneous abscess in 9 out of 10 mice, whereas those in TPS-1 medium produced abscesses in 2 out of 10 mice. In SDS-PAGE, trichomonad lysates from both media showed ten common bands. However, trichomonads in TYM medium showed additional bands of 136 kDa, 116 kDa and 40 kDa in comparison to those in TPS-1 with 100 kDa. By immunoblot with T. vaginalis-immunized rabbit sera, T. vaginalis cultivated in both TYM and TPS-1 media showed 5 common bands, and unique bands of 116 kDa, 105 kDa, and 86 kDa were observed in trichomonads in TYM while a 140 kDa band in those in TPS-1. In gelatin SDS-PAGE, trichomonads in TYM degraded gelatin stronger than those in TPS-1. Also protease activity of trichomonads in TYM was significantly higher than that of trichomonads in TPS-1 using Bz-Pro-Phe-Arg-Nan as a substrate. According to the results, it is assumed that the shift from TPS-1 into TYM medium for cultivation of T. vaginalis might modulate the biological and biochemical properties of T. vaginalis in vitro. Citations Citations to this article as recorded by Inhibitory effect of bee venom on the growth of Trichomonas vaginalis Ji-Hae Kim, Jae-Sook Ryu, Mi-Young Lee Toxicology and Environmental Health Sciences.2014; 6(1): 48. CrossRef The Dimension of Trichomonas vaginalis as Measured by Scanning Electron Microscopy Sang-Hoon Cheon, Seung Ryong Kim, Hyun-Ouk Song, Myoung-Hee Ahn, Jae-Sook Ryu The Korean Journal of Parasitology.2013; 51(2): 243. CrossRef Growth kinetics, antigen profiling, and proteinase activity of Egyptian Trichomonas tenax isolates derived from patients having oral infections Mahmoud M. El Sibaei, Nashwa S. Abdel-Fattah, Sabah A. Ahmed, Hanan M. Abou-Seri Experimental Parasitology.2012; 130(4): 416. CrossRef Phenotypic ‘variant’ forms of Trichomonas vaginalis trophozoites from cervical neoplasia patients Afzan M. Yusof, Suresh Kumar Experimental Parasitology.2012; 131(3): 267. CrossRef 7,408 View 74 Download Crossref