đŸ‘€ F. Siu

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Also published as: K.K.W. Siu, Y. A. Siu
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S. Hangan, J. Lodge, A. Odani +529 more · 2024 · Molecules · MDPI · added 2026-04-20
S. Hangan, J. Lodge, A. Odani, T. Yamaguchi, I. Persson, N. Hadjiliadis, E. Sletten, S.A. Mehrdad, A. Cucchiarini, J.L. Mergny, S.K. Noureini, S. Muthaiah, A. Bhatia, M. Kannan, A.N. Srivastva, M. Stankovic, J. Kljun, N.L.J. Stevanovic, J. Lazic, S.S. Bogojevic, S. Vojnovic, M. Zlatar, J. Nikodinovic-Runic, I. Turel, M.I. Djuran, I. Aleksic, A. Veselinovic, B.D. Glisic, H. Alshater, A.I. Al-Sulami, S.A. Aly, E.M. Abdalla, M.A. Sakr, S.S. Hassan, S. de la Mata Moratilla, S. Casado Angulo, N. GĂłmez-Casanova, J.L. Copa-Patiño, I. Heredero-Bermejo, F.J. de la Mata, S. GarcĂ­a-Gallego, A. Hangan, A. Turza, R.L. Lucaciu, B. Sevastre, E. Pall, L.S. Oprean, G. Borodi, D. Rusu, A. Stănilă, I.O. Marian, C.O. Marian, M. Rusu, R. Lucaciu, T.J. Hubin, P.N. Amoyaw, K.D. Roewe, N.C. Simpson, R.D. Maples, T.N. Carder Freeman, A.N. Cain, J.G. Le, S.J. Archibald, S.I. Khan, E. Bortolamiol, F. Visentin, T. Scattolin, I. Kostova, A.C. Hangan, L. Dican, E. PĂĄll, R.L. Stan, S. Gheorghe-Cetean, A. Tsoupras, S. Pafli, C. Stylianoudakis, K. Ladomenou, C.A. Demopoulos, A. Philippopoulos, J. Wlodarczyk, J. Krajewska, L. Szeleszczuk, P. Szalwinska, A. Gurba, S. Lipiec, P. Taciak, R. Szczepaniak, I. Mlynarzuk-Bialy, J. Fichna, C. Abate, F. Carnamucio, O. Giuffre, C. Foti, C. Chuong, C.M. DuChane, E.M. Webb, P. Rai, J.M. Marano, C.M. Bernier, J.S. Merola, J. Weger-Lucarelli, L. Oprean, P. Kumar, S. Gorai, M.K. Santra, B. Mondal, D. Manna, M. Sirajuddin, S. Ali, A. Badshah, J.D. Watson, F.H.C. Crick, B. Maddox, P.J. Kennelly, K.M. Botham, O. McGuinness, V.W. Rodwell, P.A. Weil, R.A. Harvey, D.R. Ferrier, J.M. Berg, J.L. Tymoczko, G.J. Gatto, L. Stryer, J.A. Cowan, P. Yakovchuk, E. Protozanova, M.D. Frank-Kamenetskii, M.J. Hannon, I. Bertini, H.B. Gray, S.J. Lippard, J.S. Valentine, Z. Shakked, G. Guerstein-Guzikevich, M. Eisenstein, F. Frolow, D. Rabinovich, J.C. Garcia-Ramos, R. Galindo-Murillo, F. Cortez-Guzman, L. Ruiz-Azuara, S. Neidle, M. HĂ€gerlöf, P. Papsai, C.S. Chow, S.K.C. Elmroth, J. François, N.T. Thuong, C. HĂ©lĂšne, J.L. Huppert, T.A. Brooks, S. Kendrick, L. Hurley, X. Li, Y. Peng, J. Ren, X. Qu, Y. Akiyama, S.M. Hecht, L.H. Hurley, J. Zhou, C. Wei, G. Jia, X. Wang, Z. Feng, C. Li, A. Mukherjee, K.M. Vasquez, E. Marian, L.G. Vicas, J. Tunde, M. Muresan, Z. Diaconeasa, C. Ionescu, R.G. Pearson, G. Barone, A. Terenzi, A. Lauria, A.M. Almerico, J.M. Leal, N. Busto, B. Garcia, J. Vinje, J.A. Parkinson, P.J. Sadler, T. Brown, A.A. Almaqwashi, T. Paramanathan, I. Rouzina, M.C. Williams, F.R. Keene, J.A. Smith, J.G. Collins, A. Rilak, R. Masnikosa, I. Bratsos, E. Alessio, S.K. Srivastava, T.C. Johnstone, K. Suntharalingam, S. Cetean, T. Ciuleanu, D.C. Leucuta, C. Cainap, A.M. Constantin, I. Cazacu, S. Cainap, A. Gherman, Y. He, Y. Ding, D. Wang, W. Zhang, W. Chen, X. Liu, W. Qin, X. Qian, H. Chen, Z. Guo, E. StefĂ no, F. De Castro, A. Ciccarese, A. Muscella, S. Marsigliante, M. Benedetti, F.P. Fanizzi, P.M. Takahara, A.C. Rosenzweig, C.A. Frederick, M. Demeunynck, C. Bailly, W.D. Wilson, K. Nakamoto, M. Tsuboi, G.D. Strahan, B.M. Zeglis, V.C. Pierre, J.K. Barton, C. Shobha Devi, B. Thulasiram, R.R. Aerva, P. Nagababu, T. Biver, F. Secco, M. Venturini, C.E. Maciel-Flores, J.A. Lozano-Alvarez, E.Y. BiviĂĄn-Castro, F. Jia, S. Wang, Y. Man, B. Liu, P. Modrich, A. Erxleben, E. Dumont, A. Monari, D.L. Morris, G.S. Khan, A. Shah, D. Zia-ur-Rehman, B.J. Pages, D.L. Ang, E.P. Wright, J.R. Aldrich-Wright, S.M. Nelson, L.R. Ferguson, W.A. Denny, L. Winkler, F. Cortes-Guzman, T.E. Cheatham, O. Sarpataki, N.K. Olah, M. Taulescu, I. Marcus, C. Cătoi, M.M. GonzĂĄlez-Ballesteros, L. SĂĄnchez-SĂĄnchez, A. Espinoza-GuillĂ©n, J. Espinal-EnrĂ­quez, C. MejĂ­a, E. HernĂĄndez-Lemus, P.H. von Hippel, A.H. Marcus, S. Komeda, T. Moulaei, K. Kruger Woods, M. Chikuma, N.P. Farrell, L.D. Williams, T. Jany, A. Moreth, C. Gruschka, A. Sischka, A. Spiering, M. Dieding, Y. Wang, S. Haji Samo, A. Stammler, H. Bögge, S. Li, B. Yuan, J. Zhang, L. Yue, H. Hou, J. Hu, S. Chen, B.R. Kirthan, M.C. Prabhakara, H.S. Bhojya Naik, P.H.A. Nayak, E.I. Naik, U. Saha, S. Chatterjee, M. Dolai, G.S. Kumar, A.M. Abu-Dief, N.H. Alotaibi, E.S. Al-Farraj, H.A. Qasem, S. Alzahrani, M.K. Mahfouz, A. Abdou, B. Kurt, H. Temel, M. Atlan, S. Kaya, H.A. Kiwaan, A.S. El-Mowafy, A.A. El-Bindary, S. Baskaran, M.N. Krishnan, M. Arumugham, R. Kumar, N. Kumar, R. Kaushal, P. Awasthi, A. Kellett, Z. Molphy, C. Slator, V. McKee, V.G. Vaidyanathan, B.U. Nair, R. Vijayalakshmi, P. Karacan, O. Okay, S. Phukan, S. Mitra, S. Nafisi, A.A. Saboury, N. Keramat, J.F. Neault, H.A. Tajmir-Riahi, P. Sathyadevi, P. Krishnamoorthy, R.R. Butorac, A.H. Cowley, N.S.P. Bhuvanesh, N. Dharmaraj, F. Arjmand, S. Parveen, M. Afzal, M. Shahid, J.B. Lepecq, C. Paoletti, J.L. Garcia-Gimenez, M. Gonzalez-Alvarez, M. Liu-Gonzalez, B. Macias, J. Borras, G. Alzuet, M. Aslanoglu, M. Zaheer, R. Qureshi, Z. Akhter, M.F. Nazar, M. Ngoepe, H. Clayton, P. Mucha, P. Hikisz, K. GwoĆșdziƄski, U. Krajewska, A. Leniart, E. Budzisz, E.F. Garman, J.R. Helliwell, E.P. Mitchell, A.N. Boynton, K.M. Boyle, M.J. Waring, S. Da Vela, D.I. Svergun, L.A. Feigin, P.P.P. Kumar, D.K. Lim, T.H. Jensen, M. Bech, O. Bunk, M. Thomsen, A. Menzel, A. Bouchet, G. Le Duc, R. Feidenhans, F. Pfeiffer, S. Sidhu, G. Falzon, S.A. Hart, J.G. Fox, R.A. Lewis, K.K.W. Siu, D.A. Jacques, J. Trewhella, N. Allec, M. Choi, N. Yesupriya, B. Szychowski, M.R. White, M.G. Kann, E.D. Garcin, M.C. Daniel, A. Badano, Y. Qu, J.B. Mangrum, A. Hegmans, S.J. Berners-Price, L. Ronconi, X. Filip, C. Tripon, C. Morari, C. Filip, T. Urathamakul, D.J. Waller, J.L. Beck, S.F. Ralph, X. Fan, J. Wang, X. Zhang, Z. Yang, J.C. Zhang, L. Zhao, H. Peng, J. Lei, H.W. Wang, J.L. Rubinstein, X. Benjin, L. Ling, A. Punjani, D.J. Fleet, M.A. Brubaker, A. Goldstein, Y. Soroka, M. FruĆĄic-Zlotkin, I. Popov, R. Kohen, M. Havrdova, K. Polakova, J. Skopalik, M. Vujtek, A. Mokdad, M. Homolkova, J. Tucek, J. Nebesarova, R. Zboril, M. Malatesta, M.R. RodrĂ­guez, M.J. Lavecchia, B.Z. ParajĂłn-Costa, A.C. GonzĂĄlez-BarĂł, M.R. GonzĂĄlez-BarĂł, E. CattĂĄneo, A.N. Alaghaz, S. Aldulmani, A. Yadav, K. Poonia, R. Ștefan, K.R. Fox, M.V. Villa, R. Lapresa, J. Hernandez-Gil, F. Sanz, J.B. Chaires, M. Mudasir, E.T. Wahyuni, D.H. Tjahjono, N. Yoshioka, H. Inoue, P. Jaividhya, R. Dhivya, M.A. Akbarsha, M. Palaniandavar, N. Raman, R. Jeyamurugan, A. Sakthivel, L. Mitu, A. Prisecaru, R.G. Kipping, E.J. Peterson, J.L. GarcĂ­a-GimĂ©nez, J. HernĂĄndez-Gil, A. MartĂ­nez-RuĂ­z, A. Castiñeiras, M. Liu-GonzĂĄles, F.V. PallardĂł, J. BorrĂĄs, G. Alzuet Piña, M. Swathi, D.S. Shankar, S. Daravath, N. Ganji, P.V.A. Lakshmi, R. Shivaraj, A. PĂ©rez, F.J. Luque, M. Orozco, N.M. Henriksen, D.R. Davis, D.A. Case, T.E.I. Cheatham, T. Darden, H. Gohlke, R. Luo, K.M. Merz, A. Onufriev, C. Simmerling, B. Wang, R.J. Woods, M.B. Peters, Y. Yang, L. FĂŒsti-MolnĂĄr, M.N. Weaver, M. Sahadevan, M. Sundaram, K. Subramanian Show less
DNA structure has many potential places where endogenous compounds and xenobiotics can bind. Therefore, xenobiotics bind along the sites of the nucleic acid with the aim of changing its structure, its Show more
DNA structure has many potential places where endogenous compounds and xenobiotics can bind. Therefore, xenobiotics bind along the sites of the nucleic acid with the aim of changing its structure, its genetic message, and, implicitly, its functions. Currently, there are several mechanisms known to be involved in DNA binding. These mechanisms are covalent and non-covalent interactions. The covalent interaction or metal base coordination is an irreversible binding and it is represented by an intra-/interstrand cross-link. The non-covalent interaction is generally a reversible binding and it is represented by intercalation between DNA base pairs, insertion, major and/or minor groove binding, and electrostatic interactions with the sugar phosphate DNA backbone. In the present review, we focus on the types of DNA–metal complex interactions (including some representative examples) and on presenting the methods currently used to study them. Show less
📄 PDF DOI: 10.3390/molecules29184361
DNA-binding coordination-chemistry review
R.R. Zhou, C. Alarcón, C. Nadal +374 more · 2021 · Cancers · MDPI · added 2026-04-20
R.R. Zhou, C. Alarcón, C. Nadal, C. Van Poznak, J. Massagué, J.M. Angelastro, P.D. Canoll, J. Kuo, M. Weicker, A. Costa, J.N. Bruce, L. A Greene, R. Piva, E. Pellegrino, M. Mattioli, L. Agnelli, L. Lombardi, F. Boccalatte, G. Costa, B.A. Ruggeri, M. Cheng, R. Chiarle, S.E. Monaco, M. Szabolcs, L.A. Greene, W.J. Oh, V. Rishi, A. Orosz, M.J. Gerdes, C. Vinson, Z. Sheng, L. Li, L.J. Zhu, T.W. Smith, A. Demers, A.H. Ross, R.P. Moser, M.R. Green, M.S. Carro, W.K. Lim, M.J. Alvarez, R.J. Bollo, X. Zhao, E.Y. Snyder, E.P. Sulman, S.L. Anne, F. Doetsch, H. Colman, J. Rousseau, V. Gagné, M. Labuda, C. Beaubois, D. Sinnett, C. LaverdiÚre, A. Moghrabi, S.E. Sallan, L.B. Silverman, D. Neuberg, T.R. Sarkar, S. Sharan, J. Wang, S.A. Pawar, C.A. Cantwell, P.F. Johnson, D.K. Morrison, J.-M. Wang, E. Sterneck, M. Hu, B. Wang, D. Qian, L. Zhang, X. Song, D.X. Liu, Y.-H. Wang, W.-J. Wu, W.-J. Wang, H.-Y. Huang, W.-M. Li, B.-W. Yeh, T.-F. Wu, Y.-L. Shiue, J.J.-C. Sheu, S. Ishihara, M. Yasuda, A. Ishizu, M. Ishikawa, H. Shirato, H. Haga, A. Nukuda, H. Endoh, T. Mizutani, K. Kawabata, S. Banerjee, N. Aykin-Burns, K.J. Krager, S.K. Shah, S.B. Melnyk, M. Hauer-Jensen, J.D. Gardiner, L.M. Abegglen, X. Huang, B.E. Carter, E.A. Schackmann, M. Stucki, C.N. Paxton, R.L. Randall, J.F. Amatruda, A.R. Putnam, Y. Zhang, H.-R. Wang, J.L. Wrana, S. Ben-Shmuel, R. Rashed, R. Rostoker, E. Isakov, Z. Shen-Orr, D. Leroith, C.-F. Li, Y.-Y. Chu, T.-C. Hour, C.-J. Yen, W.-C. Chang, Z.J. Messenger, J.R. Hall, D.D. Jima, J.S. House, H.W. Tam, D.A. Tokarz, R.C. Smart, D. Liu, X.-X. Zhang, M.-C. Li, C.-H. Cao, D.-Y. Wan, B.-X. Xi, J.-H. Tan, Z.-Y. Yang, X.-X. Feng, J. Feldheim, A.F. Kessler, D. Schmitt, L. Wilczek, T. Linsenmann, M. Dahlmann, C.M. Monoranu, R.-I. Ernestus, C. Hagemann, M. Löhr, F. Wang, Y. Gao, L. Tang, K. Ning, N. Geng, H. Zhang, Y. Li, F. Liu, F. Li, Q. Du, Z. Tan, F. Shi, M. Tang, L. Xie, L. Zhao, J. Hu, M. Zhou, A. Bode, D. Wang, X. Cheng, M. Guo, W. Zhao, J. Qiu, Y. Zheng, M. Meng, X. Ping, X. Chen, X. Ruan, X. Liu, Y. Xue, L. Shao, C. Yang, L. Zhu, Y. Yang, Z. Li, B. Yu, H. Wu, J. Gu, D. Zhou, W. Cheng, Y. Wang, Q. Wang, X. Wang, T. Kudo, M.T. Prentzell, S.R. Mohapatra, F. Sahm, Z. Zhao, I. Grummt, W. Wick, C.A. Opitz, M. Platten, E.W. Green, Z.-Y. Hua, J.N. Hansen, M. He, S.-K. Dai, Y. Choi, M.D. Fulton, S.M. Lloyd, M. Szemes, J. Sen, H.-F. Ding, A. Arias, M.W. Lamé, L. Santarelli, R. Hen, C.C. Cates, A.D. Arias, L.S.N. Wong, M. Sidorov, G. Cayanan, D.J. Rowland, J. Fung, G. Karpel-Massler, M.D. Siegelin, B.A. Horst, C. Shu, L. Chau, T. Tsujiuchi, P. Canoll, X. Sun, P. Jefferson, Q. Zhou, M. Olive, S.C. Williams, C. Dezan, A.W. Reinke, J. Baek, O. Ashenberg, A.E. Keating, C.R. Vinson, T. Hai, S.M. Boyd, E. Dupont, A. Prochiantz, A. Joliot, A.M. Sonabend, J. Yun, L. Lei, R. Leung, C. Soderquist, C. Crisman, B.J. Gill, A. Carminucci, J. Sisti, M. Castelli, J.-F. Beaulieu, D. Ménard, W. Chai, I. Ullah, K. Chung, S. Bae, C. Kim, B. Choi, H.Y. Nam, S.H. Kim, C.-O. Yun, K.Y. Lee, S. Rodrigues-Ferreira, H. Moindjie, M.M. Haykal, C. Nahmias, R. Xu, Z. Ji, C. Xu, J. Zhu, N.J. Caron, S.P. Quenneville, J.P. Tremblay, S.Y. Van Der Zanden, X. Qiao, J. Neefjes, F. A Fornari, W.D. Jarvis, S. Grant, M.S. Orr, J.K. Randolph, F.K. White, V.R. Mumaw, E.T. Lovings, R.H. Freeman, D. A Gewirtz, A. Bojko, J. Czarnecka-Herok, A. Charzynska, M. Dabrowski, E. Sikora, T. Kuilman, C. Michaloglou, L.C. Vredeveld, S. Douma, R. Van Doorn, C.J. Desmet, L.A. Aarden, W.J. Mooi, D.S. Peeper, E.S. Hungness, G.-J. Luo, T.A. Pritts, B.W. Robb, D. Hershko, P.-O. Hasselgren, M.Y. Taher, D.M. Davies, J. Maher, J. David, C. Dominguez, D.H. Hamilton, C. Palena, J. Al Sarraj, G. Thiel, F. Siu, C. Chen, C. Zhong, M.S. Kilberg, M. Chiu, G. Taurino, M.G. Bianchi, O. Bussolati, S.P. Wheatley, D.C. Altieri, N.M. Warrier, P. Agarwal, P. Kumar, D.M. García, N. Manero-Rupérez, R. Quesada, L. Korrodi-Gregório, V. Soto-Cerrato, D. Merino, D. Dluzen, G. Li, D. Tacelosky, M. Moreau, W. Li, C. Fiorese, A.M. Schulz, Y.-F. Lin, N. Rosin, M.W. Pellegrino, C.M. Haynes, B. Madarampalli, Y. Yuan, K. Lengel, Y. Xu, J. Yang, Z. Lu, I.K. Mann, R. Chatterjee, J. Zhao, X. He, M.T. Weirauch, T.R. Hughes, M.A. Summers, M.M. McDonald, P.I. Croucher, S.-Y. Park, J.-S. Nam, K.J. Kurppa, Y. Liu, C. To, T. Zhang, M. Fan, A. Vajdi, E.H. Knelson, Y. Xie, K. Lim, P. Cejas Show less
Simple Summary The gene-regulatory factors ATF5, CEBPB and CEBPD promote survival, growth, metastasis and treatment resistance of a range of cancer cell types. Presently, no drugs target all three at Show more
Simple Summary The gene-regulatory factors ATF5, CEBPB and CEBPD promote survival, growth, metastasis and treatment resistance of a range of cancer cell types. Presently, no drugs target all three at once. Here, with the aim of treating cancers, we designed novel cell-penetrating peptides that interact with and inactivate all three. The peptides Bpep and Dpep kill a range of cancer cell types in culture and in animals. In animals with tumors, they also significantly increase survival time. In contrast, they do not affect survival of non-cancer cells and have no apparent side effects in animals. The peptides work in combination with other anti-cancer treatments. Mechanism studies of how the peptides kill cancer cells indicate a decrease in survival proteins and increase in death proteins. These studies support the potential of Bpep and Dpep as novel, safe agents for the treatment of a variety of cancer types, both as mono- and combination therapies. Abstract Transcription factors are key players underlying cancer formation, growth, survival, metastasis and treatment resistance, yet few drugs exist to directly target them. Here, we characterized the in vitro and in vivo anti-cancer efficacy of novel synthetic cell-penetrating peptides (Bpep and Dpep) designed to interfere with the formation of active leucine-zipper-based dimers by CEBPB and CEBPD, transcription factors implicated in multiple malignancies. Both peptides similarly promoted apoptosis of multiple tumor lines of varying origins, without such effects on non-transformed cells. Combined with other treatments (radiation, Taxol, chloroquine, doxorubicin), the peptides acted additively to synergistically and were fully active on Taxol-resistant cells. The peptides suppressed expression of known direct CEBPB/CEBPD targets IL6 , IL8 and asparagine synthetase ( ASNS ), supporting their inhibition of transcriptional activation. Mechanisms by which the peptides trigger apoptosis included depletion of pro-survival survivin and a required elevation of pro-apoptotic BMF. Bpep and Dpep significantly slowed tumor growth in mouse models without evident side effects. Dpep significantly prolonged survival in xenograft models. These findings indicate the efficacy and potential of Bpep and Dpep as novel agents to treat a variety of cancers as mono- or combination therapies. Show less
📄 PDF DOI: 10.3390/cancers13102504