123487-55-8Relevant articles and documents
Total synthesis of the fully lipidated glycosylphosphatidylinositol (GPI) anchor of malarial parasite Plasmodium falciparum
Ali, Asif,Vishwakarma, Ram A.
scheme or table, p. 4357 - 4369 (2010/07/06)
We report a new and convergent strategy for the total synthesis of fully lipidated glycosylphosphatidylinositol (GPI) anchor, the major pro-inflammatory factor of malarial parasite (Plasmodium falciparum). The key features of our approach include, the acc
Efficient chemical synthesis of a dodecasaccharidyl lipomannan component of mycobacterial lipoarabinomannan
Fraser-Reid, Bert,Chaudhuri, Siddharfha Ray,Jayaprakash,Lu, Jun,Ramamurty, Changalvala V. S.
scheme or table, p. 9732 - 9743 (2009/04/06)
(Chemical Equation Presented) Lipomannan (LM) is one of the domains of lipoarabinomannan (LAM) glycolipids, the latter being one of several cell surface organic molecules that fortify mycobacterial species against external attack. Some members of mycobacterial families are pathogenic, most notably Mycobacterium tuberculosis and Mycobacterium leprae, while others are nonpathogenic, and used in the clinic, such as Mycobacterium smegmatis. Additional biological significance arises from the fact that LM has been implicated in several health disorders outside of those associated with mycobacterial pathogens, notably for treatment of bladder cancer. LM is comprised of a heavily lipidated phosphoinositide dimannoside headgroup, from which a mannan array, of varied complexity, extends. The latter consists of a 1,6-α-linked backbone flanked at position O2, not necessarily regularly, with α-linked mannosides. This paper gives an example of lipomannan synthesis in which all of the sugar components, whether functioning as donors or acceptors, are obtained from n-pentenyl orthoesters, themselves in turn prepared in three easy steps from D-mannose. Assembly of the mannan array is facilitated by the exquisite regioselectivity occasioned by the use of ytterbium triflate/N-iodosuccinimide as the trigger for reaction of n-pentenyl orthoesters.
Ionic liquid [bmim]PF6-mediated synthesis of 1,2-orthoesters of carbohydrates and the glycosidation reactions of 4-pentenyl orthoesters
Anas, Saithalavi,Sajisha, Valiyaveetil Sanjayan,Rajan, Rani,Kumaran, Rajasekaran Thirumalai,Radhakrishnan, Kokkuvayil Vasu
, p. 553 - 560 (2008/02/11)
A facile synthesis of the 1,2-orthoesters of carbohydrates in the ionic liquid [bmim]PF6 without a quaternary ammonium salt like tetrabutylammonium iodide, is described. The glycosidation reactions of 4-pentenyl orthoesters (NPOEs) with differe
A new approach to construct full-length glycosylphosphatidylinositols of parasitic protozoa and [4-deoxy-Man-III]-GPI analogues
Ali, Asif,Gowda, D. Channe,Vishwakarma, Ram A.
, p. 519 - 521 (2008/09/18)
A new [2 + 2 + 2] approach to construct GPI molecules through the efficient synthesis of glucosamine-inositol and tetramannose intermediates led to a total synthesis of a GPI-anchor of Trypanosoma cruzi, and also afforded a key intermediate for the synthe
A facile and eco-friendly method for the synthesis of 1,2-orthoesters of carbohydrates in ionic liquid
Radhakrishnan,Sajisha,Chacko, Jessy Maria
, p. 997 - 999 (2007/10/03)
A facile method for the synthesis of 1,2-orthoesters of carbohydrates in ionic liquid [bmim]PF6 is described. The method described herein is simpler, eco-friendly and avoids the addition of quaternary ammonium salts as promoters.
One-pot chemo-, regio-, and stereoselective double-differential glycosidation mediated by lanthanide triflates
Jayaprakash,Fraser-Reid, Bert
, p. 4211 - 4214 (2007/10/03)
(Chemical Equation Presented) Nuanced activation of n-pentenyl, thioglycoside, and trichloroacetimidate donors by lanthanide salts coupled with donor/acceptor matching can simplify oligosaccharide assembly. Thus, a one-pot, double-differential glycosidati
Comparing n-pentenyl orthoesters and n-pentenyl glycosides as alternative glycosyl donors
Mach, Mateusz,Schlueter, Urs,Mathew, Felix,Fraser-Reid, Bert,Hazen, Kevin C
, p. 7345 - 7354 (2007/10/03)
As is well known, cyclic 1,2-glycosyl orthoesters undergo ready acid catalyzed rearrangement to 2-O-acyl glycosides in which the alkoxy group is transferred from the orthoester to the anomeric center in a highly stereocontrolled process. The related n-pentenyl derivatives are unique in that either the orthoester (NPOE) or its rearrangement product (NPGAC) can function as a glycosyl donor, and mechanistic considerations indicate that both should (or could!) lead to the same product(s) arising from trans-orthoesterification, glycosidation, glycosyl esterification, etc. Experiments are described which show that the product obtained from a given reaction can be optimized by careful choice of the donor, NPOE or related NPGAC, and careful attention to reaction conditions, electrophilic promoter, 'size' of the glycosyl acceptor, and experimental protocol.
Studies related to synthesis of glycophosphatidylinositol membrane-bound protein anchors. 5. n-pentenyl ortho esters for mannan components
Roberts, Carmichael,Madsen, Robert,Fraser-Reid, Bert
, p. 1546 - 1553 (2007/10/02)
Procedures for rapid assembly of multigram amounts of mannan components have been examined. Although these studies are reported in the context of the mannan moiety of the glycan anchors of membrane-bound glycoproteins, the procedures should be applicable
