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The Synthesis And Biological Evaluation Of Structurally Simplified Bryostatin Analogues And The Total Synthesis Of Swinholide A
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Book Synopsis The Synthesis and Biological Evaluation of Structurally Simplified Bryostatin Analogues and the Total Synthesis of Swinholide A by : Matthew Brian Kraft
Download or read book The Synthesis and Biological Evaluation of Structurally Simplified Bryostatin Analogues and the Total Synthesis of Swinholide A written by Matthew Brian Kraft and published by . This book was released on 2011 with total page 396 pages. Available in PDF, EPUB and Kindle. Book excerpt:
Book Synopsis The Design, Synthesis, and Biological Evaluation of Structurally Simplified Bryostatin and Laulimalide Analogues by : Michael Kenneth Hilinski
Download or read book The Design, Synthesis, and Biological Evaluation of Structurally Simplified Bryostatin and Laulimalide Analogues written by Michael Kenneth Hilinski and published by . This book was released on 2006 with total page 682 pages. Available in PDF, EPUB and Kindle. Book excerpt:
Book Synopsis Efficient Access to Functional Bryostatin Analogs by : Brian Andrew Loy
Download or read book Efficient Access to Functional Bryostatin Analogs written by Brian Andrew Loy and published by . This book was released on 2013 with total page pages. Available in PDF, EPUB and Kindle. Book excerpt: The marine-derived bryostatin family of natural products represents a structurally complex molecular scaffold that has inspired a large body of synthetic and mechanistic research relevant to a number of human disease indications. Interest in the therapeutic use of bryostatin began in 1968 following a report by Pettit and coworkers that an organic extract from Bugula neritina demonstrated anticancer activity. Since its subsequent isolation and structural characterization in 1982, bryostatin has garnered increasing attention from synthetic chemists, biologists, and clinicians due to both its inherent molecular complexity as well as the wide variety of biological activities this natural product has exhibited. Bryostatin has demonstrated several anticancer activities including the promotion of apoptosis, reversal of multidrug resistance, stimulation of the immune system, and synergism with other oncolytic agents. As a result of this astounding biological activity, bryostatin 1 has been evaluated in over 30 Phase I and II clinical trials for anticancer treatment, primarily in combination with other anticancer therapeutics. Bryostatin has more recently proven capable of enhancing memory and learning in several animal models, attributable in part to its ability to induce the formation of new synaptic contacts in the brain. Bryostatin has also exhibited neuroprotective effects in animal models of cerebral ischemia. This collection of impressive neurological activities suggests a potential therapeutic use of bryostatin in the treatment of stroke, Alzheimer's disease, and other neurodegenerative disorders. Indeed, a Phase II clinical trial to explore the use of bryostatin in the treatment of Alzheimer's disease has been opened. Even more recently, bryostatin has been reported to activate latent HIV reservoirs, providing a potential first-in-class strategy for the eradication of HIV/AIDS. Unfortunately, the low natural abundance of the bryostatins from their natural source or from biological and total synthetic efforts has limited their availability for further preclinical and clinical research and development. To circumvent issues related to the supply problem of bryostatin, while providing opportunities for improved therapeutic function, the Wender research group has focused upon the design and synthesis of structurally-simplified, step-economical bryostatin analogs that exhibit biological activities comparable or superior to the natural product. This strategy, dubbed "function-oriented synthesis" (FOS), relies upon recapitulation of the biologically-active lead structure on a simplified scaffold, retaining elements necessary for function, while simplifying or eliminating those that are functionally unnecessary, thereby rendering the target more readily accessible through chemical synthesis. Application of this approach has resulted in the synthesis of a library of over 100 bryostatin analogs, the most promising of which are currently undergoing preclinical investigation for their use in the treatment of cancer, Alzheimer's disease, and the activation of latent HIV reservoirs. Chapter 1 provides the background and justification for the remainder of the dissertation. A brief overview of the bryostatins, their potent biological activities, and an in-depth discussion of the various biological and total synthetic efforts aimed at their access is provided for context. Also included is a description of the pharmacophore hypothesis first advanced by our group in 1988, and its application in in the design and synthesis of non-natural functional bryostatin analogs. The general synthetic routes utilized to access these simplified bryostatin analogs is included, as well as a brief description of the biological activities and preclinical investigation of these agents. Chapter 2 provides a review on the principal intracellular target of the bryostatins, protein kinase C (PKC). In addition to an overview of its primary structure, a detailed discussion is provided of the published structural studies of the PKC C1 binding domain, how these studies have aided in determining how our designed analogs might interact with PKC, and a brief discussion of the shortcomings of these studies. Chapters 3 and 4 detail the design and synthesis of a family of novel peripherally-functionalized bryostatin analogs. Preliminary observations suggested that the design of highly simplified analogs lacking functionalization around the northern periphery of the bryostatin scaffold might be an oversimplification, and that A-ring functionality in particular could be utilized to modulate PKC selectivity. A library of diversified A-ring functionalized analogs was designed to further probe the role of peripheral functionalities upon PKC affinity and selectivity. While each analog displayed a potent binding affinity for PKC, this collection of analogs covered a range of selectivities in which some members emulated the PKC functional selectivity of the natural product, bryostatin 1, whereas others exhibited complementary functional selectivities. In addition to these preliminary results, Chapter 4 presents the evaluation of a subset of these analogs in several in vitro and ex vivo assays relevant to HIV/AIDS eradication efforts. These simplified bryostatin analogs demonstrated a potent ability to activate latent HIV viral reservoirs without the concomitant toxic production of high levels of proinflammatory cytokines. In addition, these analogs exhibited the ability to downregulate the expression of CD4, CCR5, and CXCR4 cell surface receptors, indicating that they may help inhibit de novo infection of healthy cells. Finally, these analogs efficiently induced viral reactivation in ex vivo samples isolated from HIV-infected patients on viral suppressive therapy, indicating for the first time that simplified analogs of bryostatin function as desired in the ultimate target of HIV eradication efforts. Finally, Chapter 5 provides an introduction to an exciting collaboration that has been established between the Wender and Cegelski research groups directed at the first experimental determination of the bryostatin binding conformation when bound to PKC in a phospholipid membrane environment using rotational-echo double-resonance (REDOR) solid-state NMR. This project brings together several different areas from computational modeling, target design, chemical synthesis, biosynthesis, biological activity assays, and solid-state NMR. Included in this chapter is the design and synthesis of a novel series of isotopically labeled bryostatin analogs, as well as preliminary solid-state NMR results.
Book Synopsis The Total Synthesis and Biological Evaluation of Bryostatin 1 and Its Analogues by : Yam Bahadur Poudel
Download or read book The Total Synthesis and Biological Evaluation of Bryostatin 1 and Its Analogues written by Yam Bahadur Poudel and published by . This book was released on 2011 with total page 534 pages. Available in PDF, EPUB and Kindle. Book excerpt:
Book Synopsis The Design, Syntheis, and Preliminary Biological Evaluation of Structurally Simplified Bryostatin Analogs by : Joshua Courtney Hora
Download or read book The Design, Syntheis, and Preliminary Biological Evaluation of Structurally Simplified Bryostatin Analogs written by Joshua Courtney Hora and published by . This book was released on 2005 with total page 342 pages. Available in PDF, EPUB and Kindle. Book excerpt:
Book Synopsis Efficient Access to Bryostatin and Functional Bryostatin Analogs by : Adam James Schrier
Download or read book Efficient Access to Bryostatin and Functional Bryostatin Analogs written by Adam James Schrier and published by . This book was released on 2011 with total page pages. Available in PDF, EPUB and Kindle. Book excerpt: The bryostatins are a family of structurally complex natural products isolated from the marine bryozoan Bugula neritina. Bryostatin 1 is currently being investigated for cancer, Alzheimer's and HIV/AIDS indications. Despite these remarkable activities, research on the bryostatins is hampered by their low natural abundance. Efficient access by total chemical synthesis has been in large part precluded by the bryostatins' structural complexity. This dissertation describes the design, synthesis, and preliminary biological evaluation of functional bryostatin analogs that possess biological activities comparable or superior to the natural product. These fully synthetic analogs were convergently assembled in a uniquely step-economical manner using novel macrocyclization strategies, including macroacetalization and Prins-driven macrocyclization approaches. Bryostatin analogs were identified that possess unique affinities (subnanomolar) and selectivities for protein kinase C (PKC). Synthetic bryostatin analogs also exhibit subnanomolar antileukemic activity in in vitro assays. The convergent total synthesis of bryostatin 9, a highly potent congener of the natural product family, is also described.
Book Synopsis Scalable Total Synthesis of Bryostatin 1 Enables the Design, Synthesis, and Biological Evaluation of Bryostatin Analogs by : Clayton Thomas Hardman
Download or read book Scalable Total Synthesis of Bryostatin 1 Enables the Design, Synthesis, and Biological Evaluation of Bryostatin Analogs written by Clayton Thomas Hardman and published by . This book was released on 2020 with total page pages. Available in PDF, EPUB and Kindle. Book excerpt: Bryostatin 1 is a natural product that was originally isolated from the marine sponge Bugula neritina more than 50 years ago. Following its isolation, it has demonstrated unprecedented clinical potential across a number of indications, including HIV/AIDS eradication, the treatment of Alzheimer's disease and neurological disorders, and cancer immunotherapy. Despite this unique portfolio of indications, the natural supply of bryostatin 1 from its source organism is limited and variable and maintaining a consistent supply of the natural product has hindered its clinical advancement. To enable the continued clinical evaluation of bryostatin 1, we developed a scalable total synthesis of the natural product that can sustainably supply future clinical studies of this exciting clinical candidate. Despite its promising activity, bryostatin 1 is a marine natural product that is neither evolved nor optimized for the treatment of human disease. Historically, the scarcity of isolated material and the challenges associated with making modifications of the delicate and densely functionalized bryostatin skeleton have precluded efforts to optimize the biological activity of this natural product lead through derivatization and exploration of structure-activity relationships (SAR) around the macrocycle. Drawing on the synthetic platform we developed in our scalable synthesis of bryostatin 1, we accomplished the design, synthesis, and biological evaluation of the first close-in analogs of bryostatin 1. Using a function-oriented synthesis (FOS) strategy informed by a combination of computational and biological data surrounding bryostatin's interaction with its protein target, protein kinase C (PKC), we synthesized a series of bryostatin analogs designed to maintain PKC affinity while allowing for a systematic investigation of their biological function. By leveraging the modularity of our bryostatin 1 synthesis, we developed complementary late-stage diversification strategies that provide efficient synthetic access to parallel series of bryostatin analogs with modifications in the A- and B-rings. In agreement with our pharmacophore model, these new agents retain affinity for PKC but exhibit variable PKC translocation kinetics. We further demonstrate that select analogs potently induce increased cell surface expression of CD22, a promising target for the treatment of leukemias and lymphomas, in in vitro models of acute lymphoblastic leukemia (ALL) and AIDS-related lymphomas, highlighting the potential general use of bryostatin and bryostatin analogs for enhancing antigen-targeted cancer immunotherapies. Finally, bryostatin 1 has been shown to prevent progressive neurodegeneration in a mouse model of multiple sclerosis (MS). Working with Professors Paul Kim and Michael Kornberg at Johns Hopkins, we show that several bryostatin analogs replicate the anti-inflammatory effects of bryostatin 1 on innate immune cells in vitro and lead analog SUW133 attenuates neuroinflammation and prevents the development of MS-related neurological deficits in vivo. We further demonstrate that this activity is dependent on PKC. These findings identify bryostatin analogs as promising drug candidates for targeting innate immunity in neuroinflammation and create a platform for evaluation of synthetic PKC modulators for the treatment of MS and other neuroinflammatory diseases.
Book Synopsis The Design, Synthesis and Biological Evaluation of the First Totally Synthetic Bryostatin Analogues by : Blaise Lippa
Download or read book The Design, Synthesis and Biological Evaluation of the First Totally Synthetic Bryostatin Analogues written by Blaise Lippa and published by . This book was released on 2000 with total page 718 pages. Available in PDF, EPUB and Kindle. Book excerpt:
Book Synopsis Supply Impacting Synthesis of Bryostatin 1 and the Design, Synthesis, and Evaluation of Bryostatin 1 Analogs by : Akira Joseph Shimizu
Download or read book Supply Impacting Synthesis of Bryostatin 1 and the Design, Synthesis, and Evaluation of Bryostatin 1 Analogs written by Akira Joseph Shimizu and published by . This book was released on 2019 with total page pages. Available in PDF, EPUB and Kindle. Book excerpt: The marine derived natural product bryostatin 1 has been investigated in preclinical studies for a wide range of indications (cancer, Alzheimer's disease, HIV/AIDS eradication, multiple sclerosis, fragile X syndrome, and others). Bryostatin 1 has been evaluated in more than 40 clinical trials for three of these highly impactful indications: cancer, Alzheimer's disease, and HIV eradication. The trials in Alzheimer's disease and the eradication of HIV are ongoing, and there is a planned trial in which bryostatin 1 will act as an adjuvant to enhance CAR T cell therapy used to treat cancer. Unfortunately, the isolation of bryostatin 1 from its source organism is not economically or environmentally sustainable, placing the supply of bryostatin 1 for clinical evaluation in jeopardy. Additionally, although bryostatin 1 has impressive biologic activity, it was not evolved for human use. Bryostatin 1 has been heavily studied, but significantly less preclinical evaluation has been performed on designed bryostatin 1 analogs. These analogs have the potential to be more efficacious and have fewer off target side effects relative to the parent natural product. Prior research indicates that the putative pathway for the activity of bryostatin 1 is exogenous regulation of protein kinase C (PKC) activity. The PKC family of enzymes plays a central and complex role in both normal and diseased states. Structurally different PKC modulators have exhibited drastically different biologic activities. Further understanding how the subtle structural elements of the bryostatin 1 scaffold affect its multiple PKC mediated activities, potentially through isoform specificity or differential protein ligand orientation, could aid in the development of analog compounds with improved functional activity. This thesis details of the collaborative team effort to solve the bryostatin 1 supply problem through a step-economical and scalable total synthesis (19 longest linear sequence, 29 total steps, 4.8% yield). To reduce the number of steps in the longest linear sequence, this total synthesis convergently constructs bryostatin 1 by bringing together two similarly complex fragments late in the synthesis. This thesis focuses on the synthetic route to one of those fragments, the C-ring fragment, and the final steps in the total synthesis of bryostatin 1. The scalable nature of the bryostatin 1 total synthesis provided access to unprecedented amounts of highly complex intermediates with many of the key structural features of bryostatin 1. This thesis also describes how those intermediates were leveraged to produce a library of "close-in" analogs to bryostatin 1. These analogs were used to test hypotheses about which molecular interactions between bryostatin 1, PKC, and cellular membranes contribute to the amazing phenotypic activity of bryostatin 1. A subset of these bryostatin 1 analogs have been advanced to more complex functional assays to determine if the analogs have superior efficacy or tolerability relative to bryostatin 1.
Book Synopsis The Large Scale Synthesis of the C19 to C32 Portion of Swinholide A, the Total Synthesis of Dactylolide, and the Synthesis of a Novel Bryostatin Analogue by : Carina Cristina Sanchez
Download or read book The Large Scale Synthesis of the C19 to C32 Portion of Swinholide A, the Total Synthesis of Dactylolide, and the Synthesis of a Novel Bryostatin Analogue written by Carina Cristina Sanchez and published by . This book was released on 2005 with total page 544 pages. Available in PDF, EPUB and Kindle. Book excerpt:
Book Synopsis I. Design, Synthesis, and Biological Evaluation of New Analogs of Bryostatin ; II. Investigations Into the Mode of Action of Apoptolidin A by : Jeremy L. Baryza
Download or read book I. Design, Synthesis, and Biological Evaluation of New Analogs of Bryostatin ; II. Investigations Into the Mode of Action of Apoptolidin A written by Jeremy L. Baryza and published by . This book was released on 2005 with total page 574 pages. Available in PDF, EPUB and Kindle. Book excerpt:
Book Synopsis Synthetic Efforts Toward the Total Synthesis of Bryostatin 1 Emphasis on the C17-C27 Fragment by : Victoria Lynn Wilde
Download or read book Synthetic Efforts Toward the Total Synthesis of Bryostatin 1 Emphasis on the C17-C27 Fragment written by Victoria Lynn Wilde and published by . This book was released on 2008 with total page 294 pages. Available in PDF, EPUB and Kindle. Book excerpt:
Book Synopsis The Synthesis of the C-ring Subunit of Bryostatin 1, and the Synthesis and Biological Evaluation of Fluorescent Bryostatin Analogs by : Thomas Joseph Cummins
Download or read book The Synthesis of the C-ring Subunit of Bryostatin 1, and the Synthesis and Biological Evaluation of Fluorescent Bryostatin Analogs written by Thomas Joseph Cummins and published by . This book was released on 2015 with total page 483 pages. Available in PDF, EPUB and Kindle. Book excerpt:
Book Synopsis Contributions by : Stanford University. Department of Chemistry
Download or read book Contributions written by Stanford University. Department of Chemistry and published by . This book was released on 2005 with total page 618 pages. Available in PDF, EPUB and Kindle. Book excerpt: Contains reprints of articles published by members of the department.
Book Synopsis Towards the Total Synthesis of Azinomycin B by :
Download or read book Towards the Total Synthesis of Azinomycin B written by and published by . This book was released on 2008 with total page 408 pages. Available in PDF, EPUB and Kindle. Book excerpt:
Book Synopsis Studies Toward the Total Synthesis of Bryostatin 1 by : David Curtis Whritenour
Download or read book Studies Toward the Total Synthesis of Bryostatin 1 written by David Curtis Whritenour and published by . This book was released on 1988 with total page 608 pages. Available in PDF, EPUB and Kindle. Book excerpt:
Book Synopsis The Total Synthesis of Bryostatin 7 by : John Charles Roberts
Download or read book The Total Synthesis of Bryostatin 7 written by John Charles Roberts and published by . This book was released on 1991 with total page 338 pages. Available in PDF, EPUB and Kindle. Book excerpt:
