Literatura académica sobre el tema "Stambomycine"
Crea una cita precisa en los estilos APA, MLA, Chicago, Harvard y otros
Índice
Consulte las listas temáticas de artículos, libros, tesis, actas de conferencias y otras fuentes académicas sobre el tema "Stambomycine".
Junto a cada fuente en la lista de referencias hay un botón "Agregar a la bibliografía". Pulsa este botón, y generaremos automáticamente la referencia bibliográfica para la obra elegida en el estilo de cita que necesites: APA, MLA, Harvard, Vancouver, Chicago, etc.
También puede descargar el texto completo de la publicación académica en formato pdf y leer en línea su resumen siempre que esté disponible en los metadatos.
Artículos de revistas sobre el tema "Stambomycine"
Wang, Yongchen, Venkaiah Chintalapudi, Haraldur G. Gudmundsson, Gregory L. Challis y Edward A. Anderson. "Synthesis of the C50 diastereomers of the C33–C51 fragment of stambomycin D". Organic Chemistry Frontiers 9, n.º 2 (2022): 445–49. http://dx.doi.org/10.1039/d1qo01635k.
Texto completoSong, Lijiang, Luisa Laureti, Christophe Corre, Pierre Leblond, Bertrand Aigle y Gregory L. Challis. "Cytochrome P450-mediated hydroxylation is required for polyketide macrolactonization in stambomycin biosynthesis". Journal of Antibiotics 67, n.º 1 (13 de noviembre de 2013): 71–76. http://dx.doi.org/10.1038/ja.2013.119.
Texto completoSu, Li, Laurence Hôtel, Cédric Paris, Clara Chepkirui, Alexander O. Brachmann, Jörn Piel, Christophe Jacob, Bertrand Aigle y Kira J. Weissman. "Engineering the stambomycin modular polyketide synthase yields 37-membered mini-stambomycins". Nature Communications 13, n.º 1 (26 de enero de 2022). http://dx.doi.org/10.1038/s41467-022-27955-z.
Texto completoSu, Li, Laurence Hôtel, Cédric Paris, Clara Chepkirui, Alexander O. Brachmann, Jörn Piel, Christophe Jacob, Bertrand Aigle y Kira J. Weissman. "Author Correction: Engineering the stambomycin modular polyketide synthase yields 37-membered mini-stambomycins". Nature Communications 13, n.º 1 (6 de octubre de 2022). http://dx.doi.org/10.1038/s41467-022-33524-1.
Texto completoLim, Jieyan, Venkaiah Chintalapudi, Haraldur G. Gudmundsson, Minh Tran, Alice Bernasconi, Araceli Blanco, Lijiang Song, Gregory L. Challis y Edward A. Anderson. "Synthesis of the C1–C27 Fragment of Stambomycin D Validates Modular Polyketide Synthase-Based Stereochemical Assignments". Organic Letters, 8 de septiembre de 2021. http://dx.doi.org/10.1021/acs.orglett.1c02650.
Texto completoTesis sobre el tema "Stambomycine"
Su, Li. "Generation of analogues of the anti-tumor polyketide stambomycins by genetic engineering and allied approaches". Electronic Thesis or Diss., Université de Lorraine, 2021. http://www.theses.fr/2021LORR0081.
Texto completoThe polyketide secondary metabolites of bacteria are a rich source of bioactive agents, with notable applications in anti-infective and anti-cancer therapy. However, their structures often need to be optimized in order to tailor their therapeutic and biophysical properties. The 51-membered macrolide stambomycins, among the largest of known polyketides, were recently discovered by genome mining in Streptomyces ambofaciens ATCC23877, and notably exhibit promising anti-cancer activity. The family encompasses six members which differ from each other in the alkyl functionality at C-26, due to the alternative choice of extender units by an exceptional acyl transferase domain (AT12) of the modular polyketide synthase (PKS) responsible for synthesizing the stambomycin core. Given their enormous size of the stambomycins and the intrinsic promiscuity of AT12, there is substantial interest in accessing ring-contracted and C-26 substituted derivatives of this compounds which might retain the bioactivity of the parental structures, or exhibit improved or even new properties. In this work, we have leveraged our current understanding of modular PKS systems to internally contract the stambomycin assembly line, leading to the successful generation, albeit at low yield, of target smaller derivatives (37-membered ‘mini-stambomycins’). By careful analysis, we could identify multiple factors contributing to the low titers, information which should inform future engineering strategies. Furthermore, using a mutasynthesis strategy, we were able to exploit the broad specificity of the AT12 domain to create 6 novel C-26 substituted stambomycin analogues. Finally, we unexpectedly identified three series of novel desferrioxamine siderophores produced by S. ambofaciens. As a number of key metabolites generated in this work have potential interest for therapeutic applications, they will be targeted for purification, structural characterization and biological evaluation