Synthesis of α-l-rhamnosyl ceramide and evaluation of its binding with anti-rhamnose antibodies

Long, David E.; Karmakar, Partha; Wall, Kathleen; Sucheck, Steven J.

doi:10.1016/j.bmc.2014.08.002

Cited by 9 publications

(9 citation statements)

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“…9, 50, 51 In fact, Rha is now one of the most effective natural antibody eliciting molecules known 52 and Rha has been conjugated to lipids to recruit anti-Rha antibodies to tumor cells. 53, 54 …”

Section: Introductionmentioning

confidence: 99%

Synthesis of a Liposomal MUC1 Glycopeptide-Based Immunotherapeutic and Evaluation of the Effect of l-Rhamnose Targeting on Cellular Immune Responses

et al. 2015

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Generation of a CD8+ response to extracellular antigen requires processing of the antigen by antigen presenting cells (APC) and cross-presentation to CD8+ T cell receptors via MHC class I molecules. Cross-presentation is facilitated by efficient antigen uptake followed by immune-complex-mediated maturation of the APCs. We hypothesize that improved antigen uptake of a glycopeptide sequence containing a CD8+ T cell epitope could be achieved by delivering it on a liposome surface decorated with an immune complex-targeting ligand, an L-Rhamnose (Rha) epitope. We synthesized a 20 amino acid glycopeptide TSAPDT(GalNAc)RPAPGSTAPPAHGV from the variable number tandem repeat region of the tumor marker MUC1 containing an N-terminal azido moiety and a tumor-associated α-N-acetyl galactosamine (GalNAc) at the immunogenic DTR motif. The MUC1 antigen was attached to Pam3Cys, a Toll-like receptor-2 ligand via copper (I)-catalyzed azido-alkyne cycloaddtion (CuAAc) chemistry. The Rha-decorated liposomal Pam3Cys-MUC1-Tn 4 vaccine was evaluated in groups of C57BL/6 mice. Some groups were previously immunized to generate anti-Rha antibodies. Anti-Rha antibody expressing mice that received the Rha liposomal vaccine showed higher cellular immunogenicity compared to the control group while maintaining a strong humoral response.

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Section: Introductionmentioning

confidence: 99%

Synthesis of a Liposomal MUC1 Glycopeptide-Based Immunotherapeutic and Evaluation of the Effect of l-Rhamnose Targeting on Cellular Immune Responses

et al. 2015

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“…After removal of all benzoyl protecting groups by the Zemplén condition, several methods were tested to reduce the azido group while keep the alkene group intact. Methods using PPh 3 , 36 PMe 3 , 37 or Lindlar catalyst 38 led to poor yields (30–50%). The combination of 1,3-propanedithiol and triethylamine 39 were found to be the most efficient for selective reduction of the azido group to produce LacβSph ( 5 ) in an excellent yield (94%).…”

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confidence: 99%

Highly efficient chemoenzymatic synthesis and facile purification of α-Gal pentasaccharyl ceramide Galα3nLc₄βCer

Santra

et al. 2017

Chem. Commun.

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A highly efficient chemoenzymatic method for synthesizing glycosphingolipids using α-Gal pentasaccharyl ceramide as an example is reported here. Enzymatic extension of chemically synthesized lactosyl sphingosine using efficient sequential one-pot multienzyme (OPME) reactions allowed glycosylation be carried out in aqueous solution. Facile C18 cartridge-based quick (<30 minutes) purification proctols were established using minimal amounts of green solvents (CH3CN and H2O). Simple acylation in the last step led to the formation of the target glycosyl ceramide in 4 steps with an overall yield of 57%.

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“…Galα1-3Glc and Galα1-3Gal epitopes were reported on both gram-positive and gram-negative bacteria (Han et al, 2012;Lüderitz et al, 1965). Additional examples of such antibodies in humans are anti-blood group A and B antibodies (Springer and Horton, 1969), natural antibody to N-glycolylneuraminic acid (called anti-Neu5Gc), which is produced in humans, and not in other Old World primates, or in nonprimate mammals (Higashi et al, 1977;Merrick et al, 1978;Zhu and Hurst, 2002;Padler-Karavani et al, 2008), and natural anti-rhamnose antibody (Chen et al, 2011;Sheridan et al, 2014;Long et al, 2014). As detailed in Chapter 3, the reason for the ability of anti-bacterial carbohydrate antibodies to bind mammalian carbohydrate antigens is that these antibodies are polyclonal, and different clones are capable of binding to various "facets" of a given carbohydrate antigen.…”

Section: Natural Anti-carbohydrate Antibodies To Bacterial Antigensmentioning

confidence: 99%

Why Do We Produce Anti-Gal

Galili

2018

The Natural Anti-Gal Antibody as Foe Turned Friend in Medicine

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Synthesis of α-l-rhamnosyl ceramide and evaluation of its binding with anti-rhamnose antibodies

Cited by 9 publications

References 28 publications

Synthesis of a Liposomal MUC1 Glycopeptide-Based Immunotherapeutic and Evaluation of the Effect of l-Rhamnose Targeting on Cellular Immune Responses

Synthesis of a Liposomal MUC1 Glycopeptide-Based Immunotherapeutic and Evaluation of the Effect of l-Rhamnose Targeting on Cellular Immune Responses

Highly efficient chemoenzymatic synthesis and facile purification of α-Gal pentasaccharyl ceramide Galα3nLc₄βCer

Why Do We Produce Anti-Gal

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Synthesis of α-l-rhamnosyl ceramide and evaluation of its binding with anti-rhamnose antibodies

Cited by 9 publications

References 28 publications

Synthesis of a Liposomal MUC1 Glycopeptide-Based Immunotherapeutic and Evaluation of the Effect of l-Rhamnose Targeting on Cellular Immune Responses

Synthesis of a Liposomal MUC1 Glycopeptide-Based Immunotherapeutic and Evaluation of the Effect of l-Rhamnose Targeting on Cellular Immune Responses

Highly efficient chemoenzymatic synthesis and facile purification of α-Gal pentasaccharyl ceramide Galα3nLc4βCer

Why Do We Produce Anti-Gal

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Highly efficient chemoenzymatic synthesis and facile purification of α-Gal pentasaccharyl ceramide Galα3nLc₄βCer