Retargeting pre-existing human antibodies to a bacterial pathogen with an alpha-Gal conjugated aptamer

Kristian, Sascha A.; Hwang, John H.; Hall, Bradley; Leire, Emma; Iacomini, John; Old, Robert; Galili, Uri; Roberts, Charles; Mullis, Kary B.; Westby, Mike; Nizet, Victor

doi:10.1007/s00109-015-1280-4

Cited by 26 publications

(27 citation statements)

References 39 publications

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“…Retargeting pre-existing anti-α-Gal antibodies to pathogens with an alpha-Gal-conjugated aptamer could be developed as a novel therapeutic approach. 38 In addition, the recent finding that increased abundance of α-Gal producing bacteria, Lactobacillus and Bifidobacterium in the gut microbiota affects Plasmodium infection in mice. 39 This opens the possibility of using probiotics as potential interventions to reduce disease severity, which may also be conditioned by blood type in humans.…”

Section: Discussionmentioning

confidence: 99%

Effect of blood type on anti-α-Gal immunity and the incidence of infectious diseases

et al. 2017

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The identification of factors affecting the susceptibility to infectious diseases is essential toward reducing their burden on the human population. The ABO blood type correlates with susceptibility to malaria and other infectious diseases. Due to the structural similarity between blood antigen B and Galα1-3Galβ1-(3)4GlcNAc-R (α-Gal), we hypothesized that self-tolerance to antigen B affects the immune response to α-Gal, which in turn affects the susceptibility to infectious diseases caused by pathogens carrying α-Gal on their surface. Here we found that the incidence of malaria and tuberculosis, caused by pathogens with α-Gal on their surface, positively correlates with the frequency of blood type B in endemic regions. However, the incidence of dengue fever, caused by a pathogen without α-Gal, was not related to the frequency of blood type B in these populations. Furthermore, the incidence of malaria and tuberculosis was negatively correlated with the anti-α-Gal antibody protective response. These results have implications for disease control and prevention.

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Section: Discussionmentioning

confidence: 99%

Effect of blood type on anti-α-Gal immunity and the incidence of infectious diseases

et al. 2017

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“…Alpha gal antibodies also prevent organ transplantation from other mammal species – pig organs are rejected partly because they are rich in alpha gal [66]. Anti alpha gal antibodies have a potential medical applications if they could be directed against pathogens or cancerous cells [67]. …”

Section: Figurementioning

confidence: 99%

Glycomics: revealing the dynamic ecology and evolution of sugar molecules

Springer

Gagneux

2016

Journal of Proteomics

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Sugars are the most functionally and structurally diverse molecules in the biological world. Glycan structures range from tiny single monosaccharide units to giant chains thousands of units long. Some glycans are branched, their monosaccharides linked together in many different combinations and orientations. Some exist as solitary molecules; others are conjugated to proteins and lipids and alter their collective functional properties. In addition to structural and storage roles, glycan molecules participate in and actively regulate physiological and developmental processes. Glycans also mediate cellular interactions within and between individuals. Their roles in ecology and evolution are pivotal, but not well studied because glycan biochemistry requires different methods than standard molecular biology practice. The properties of glycans are in some ways convenient, and in others challenging. Glycans vary on organismal timescales, and in direct response to physiological and ecological conditions. Their mature structures are physical records of both genetic and environmental influences during maturation. We describe the scope of natural glycan variation and discuss how studying glycans will allow researchers to further integrate the fields of ecology and evolution.

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“…We chose the mouse laminin as a positive control since it is a crude glycoprotein with multiple α‐Gal epitopes. The Apt‐Lips, Lips, and mouse laminin were immobilized on 96‐well microplates and titrated by a serial dilution of hIVIG, which contains anti‐Gal antibodies . HRP conjugated anti‐human IgG antibody was used to detect the binding of anti‐Gal IgG.…”

Section: Resultsmentioning

confidence: 99%

“…The Apt-Lips, Lips, and mouse laminin were immobilized on 96-well microplates and titrated by a serial dilution of hIVIG, which contains anti-Gal antibodies. 44 HRP conjugated anti-human IgG antibody was used to detect the binding of anti-Gal IgG. As shown in Supporting Information Figure S3, human IgG had similar binding efficiency to Apt-Lips, Lips, and mouse laminins.…”

Section: Studies On the Interaction Between Human Igg And The α-Gal Lmentioning

confidence: 99%

Aptamer‐integrated α‐Gal liposomes as bispecific agents to trigger immune response for killing tumor cells

Hong

Ding

Luo

et al. 2019

J Biomedical Materials Res

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A novel bispecific α‐Gal liposome was constructed by self‐assembling AS1411 aptamers into the α‐Gal containing liposomes. The α‐Gal liposomes were prepared using cell membranes of red blood cells from rabbit, which are composed of cholesterol, phospholipids, and α‐Gal glycolipids. AS1411 is a DNA aptamer with high specificity and affinity for nucleolin and could integrate into liposomes by the modification of cholesterol. The bispecific α‐Gal liposomes surface‐functionalized by α‐Gal and AS1411 aptamer could recognize anti‐Gal antibodies and nucleolin overexpressed by tumor cells simultaneously, followed by activating the immune system to attack the tumor cells, resulting in the lysis of the tumor cells by antibody dependent cell‐mediated cytotoxicity. Under simulated tumor environment, the lysis rate of MCF‐7 cells treated by the AS1411 modified α‐Gal liposomes drastically increased compared to the liposomes without AS1411 aptamer. This study suggests that the AS1411 modified α‐Gal liposomes can recognize nucleolin‐overexpressing tumor cells selectively, subsequently improve the effect of the immunotherapy with high specificity. © 2018 Wiley Periodicals, Inc. J Biomed Mater Res Part A: 107A: 1176–1183, 2019.

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Retargeting pre-existing human antibodies to a bacterial pathogen with an alpha-Gal conjugated aptamer

Cited by 26 publications

References 39 publications

Effect of blood type on anti-α-Gal immunity and the incidence of infectious diseases

Effect of blood type on anti-α-Gal immunity and the incidence of infectious diseases

Glycomics: revealing the dynamic ecology and evolution of sugar molecules

Aptamer‐integrated α‐Gal liposomes as bispecific agents to trigger immune response for killing tumor cells

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