Your search keyword '"GXM"' showing total 6 results

1. Association Between Plasma Antibody Responses and Risk for Cryptococcus-Associated Immune Reconstitution Inflammatory Syndrome.

Author

Yoon, Hyun Ah, Nakouzi, Antonio, Chang, Christina C, Kuniholm, Mark H, Carreño, Leandro J, Wang, Tao, Ndung'u, Thumbi, Lewin, Sharon R, French, Martyn A, and Pirofski, Liise-anne

Subjects

CRYPTOCOCCUS, IMMUNE reconstitution inflammatory syndrome, HIV, MENINGITIS, IMMUNOGLOBULINS, HIV infection complications, B cells, BLOOD plasma, COMPARATIVE studies, CRYPTOCOCCUS neoformans, HIV infections, RESEARCH methodology, MEDICAL cooperation, MULTIVARIATE analysis, POLYSACCHARIDES, RESEARCH, CRYPTOCOCCOSIS, ANTIRETROVIRAL agents, EVALUATION research, ANTIBODY formation

Abstract

Background: Initiation of antiretroviral therapy (ART) in human immunodeficiency virus (HIV)-infected individuals with cryptococcal meningitis places them at risk for Cryptococcus-associated immune reconstitution inflammatory syndrome (C-IRIS). The relationship between antibody immunity and C-IRIS risk has not been investigated.Methods: We compared plasma levels of immunoglobulins, C. neoformans glucuronoxylomannan (GXM) capsule-specific and laminarin (Lam)-binding IgM and IgG, and percentages of peripheral blood total and memory B cells between 27 HIV-infected patients with CM who developed C-IRIS and 63 who did not, and evaluated associations of these parameters with risk of C-IRIS.Results: Prior to initiation of ART, plasma IgM, Lam-binding IgM (Lam-IgM), Lam-IgG, and GXM-IgM levels were significantly lower in patients who developed C-IRIS than those who did not. Multivariate analysis revealed significant inverse associations between C-IRIS and IgM (P = .0003), Lam-IgM (P = .0005), Lam-IgG (P = .002), and GXM-IgM (P = .002) independent of age, sex, HIV viral load, CD4+ T-cell count, and cerebrospinal fluid fungal burden. There were no associations between C-IRIS and total or memory B cells.Discussion: Antibody profiles that include plasma IgM, Lam-IgM, Lam-IgG, and/or GXM-IgM may have value in furthering our understanding of C-IRIS pathogenesis and hold promise as candidate biomarkers of C-IRIS risk. [ABSTRACT FROM AUTHOR]

Published

2019

2. Capsule of Cryptococcus neoformans grows by enlargement of polysaccharide molecules.

Author

Frases, Susana, Pontes, Bruno, Nimrichter, Leonardo, Viana, Nathan B., Rodrigues, Marcio L., and CasadevaII, Arturo

Subjects

CRYPTOCOCCUS, PATHOGENIC microorganisms, POLYSACCHARIDES, MICROBIAL virulence, PHARMACEUTICAL encapsulation

Abstract

The human pathogenic fungus Cryptococcus neoformans has a distinctive polysaccharide (PS) capsule that enlarges during infection. The capsule is essential for virulence, but the mechanism for capsular growth is unknown. In the present study, we used dynamic light scattering (LS) analysis of capsular PS and optical tweezers (OT) to explore the architecture of the capsule. Analysis of capsular PS from cells with small and large capsules by dynamic LS revealed a linear correlation between PS effective diameter and microscopic capsular diameter. This result implied that capsule growth was achieved by the addition of molecules with larger effective diameter, such that some molecules can span the entire diameter of the capsule. Measurement of polystyrene bead penetration of C. neoformans capsules by using OT techniques revealed that the outer regions were penetrable, but not the inner regions. Our results provide a mechanism for capsular enlargement based on the axial lengthening of PS molecules and suggest a model for the architecture of a eukaryotic microbial capsule. [ABSTRACT FROM AUTHOR]

Published

2009

3. Specification, Testing, and Interpretation of Gene-by-Measured-Environment Interaction Models in the Presence of Gene–Environment Correlation.

Author

Rathouz, Paul J., Van Hulle, Carol A., Rodgers, Joseph Lee, Waldman, Irwin D., and Lahey, Benjamin B.

Subjects

GENOTYPE-environment interaction, GENETICS, ANALYSIS of variance, BIOMETRY, BIOMATHEMATICS, RESEARCH

Abstract

Purcell (Twin Res 5:554–571, ) proposed a bivariate biometric model for testing and quantifying the interaction between latent genetic influences and measured environments in the presence of gene–environment correlation. Purcell’s model extends the Cholesky model to include gene–environment interaction. We examine a number of closely related alternative models that do not involve gene–environment interaction but which may fit the data as well as Purcell’s model. Because failure to consider these alternatives could lead to spurious detection of gene–environment interaction, we propose alternative models for testing gene–environment interaction in the presence of gene–environment correlation, including one based on the correlated factors model. In addition, we note mathematical errors in the calculation of effect size via variance components in Purcell’s model. We propose a statistical method for deriving and interpreting variance decompositions that are true to the fitted model. [ABSTRACT FROM AUTHOR]

Published

2008

4. Spleen deposition of Cryptococcus neoformans capsular glucuronoxylomannan in rodents occurs in red pulp macrophages and not marginal zone macrophages expressing the C-type lectin SIGN-R1.

Author

De Jesus, Magdia, Park, Chae Gyu, Su, Ya, Goldman, David L., Steinman, Ralph M., and Casadevall, Arturo

Abstract

The fate of microbial polysaccharides in host tissues is an important consideration because these compounds are often immune modulators. Splenic marginal zone macrophages that express the C-type lectin receptor SIGN-R1, take up neutral polysaccharides such as dextran and the capsular polysaccharide of Streptococcus pneumoniae. Given that the major component of Cryptococcus neoformans capsular polysaccharide, glucuronoxylomannan (GXM), localizes in the spleen when injected intravenously, we investigated whether GXM uptake was mediated by splenic macrophages expressing the SIGN-R1 receptor in mice. No significant differences in the amount and location of GXM deposition were detected in the spleens of mice treated with a SIGN-R1 blocking antibody when compared to controls. Similarly, a blocking antibody to Dectin-1, a co-receptor of -SIGN-R1, had no effects on GXM distribution within the spleen. Histological examination of spleens from mice and rats injected with FITC-Dextran and GXM revealed no significant co-localization, with Dextran and GXM being found in marginal and red pulp macrophages, respectively. Hence we conclude that GXM was not deposited in marginal zone macrophages. However, GXM deposition was found in the red pulp. These results indicate that there is a selective localization of these polysaccharides to different receptors such as SIGN-R1 for FITC dextran in marginal zone and a to-be-identified receptor selectively expressed by red pulp macrophages for GXM. [ABSTRACT FROM AUTHOR]

Published

2008

5. Glucuronoxylomannan exhibits potent immunosuppressive properties.

Author

Monari, Claudia, Bistoni, Francesco, Vecchiarelli, Anna, and Levitz, Stuart

Subjects

CRYPTOCOCCUS neoformans, CRYPTOCOCCUS, FUNGI, APOPTOSIS, CELL death

Abstract

Cryptococcus neoformans is an opportunistic fungus responsible for life-threatening infections in immunocompromised and occasionally in immunocompetent hosts. The fungus is endowed with several virulence factors such as its capsular polysaccharide, which plays a key role in virulence. The major component of capsular material of C. neoformans is glucuronoxylomannan, a polysaccharide that exhibits potent immunosuppressive properties in vitro and in vivo. Here we describe a new aspect relative to glucuronoxylomannan-induced immunosuppression. In this review we analyze the suppressive effects of glucuronoxylomannan and the mechanisms leading to induction of apoptosis in T cells. [ABSTRACT FROM AUTHOR]

Published

2006

6. Cryptococcus neoformans Capsular GXM Conformation and Epitope Presentation: A Molecular Modelling Study.

Author

Kuttel, Michelle M., Casadevall, Arturo, and Oscarson, Stefan

Subjects

CRYPTOCOCCUS neoformans, MOLECULAR models, MOLECULAR dynamics, IMMUNOCOMPROMISED patients, EPITOPES

Abstract

The pathogenic encapsulated Cryptococcus neoformans fungus causes serious disease in immunosuppressed hosts. The capsule, a key virulence factor, consists primarily of the glucuronoxylomannan polysaccharide (GXM) that varies in composition according to serotype. While GXM is a potential vaccine target, vaccine development has been confounded by the existence of epitopes that elicit non-protective antibodies. Although there is evidence for protective antibodies binding conformational epitopes, the secondary structure of GXM remains an unsolved problem. Here an array of molecular dynamics simulations reveal that the GXM mannan backbone is consistently extended and relatively inflexible in both C. neoformans serotypes A and D. Backbone substitution does not alter the secondary structure, but rather adds structural motifs: β DGlcA and β DXyl side chains decorate the mannan backbone in two hydrophillic fringes, with mannose-6-O-acetylation forming a hydrophobic ridge between them. This work provides mechanistic rationales for clinical observations—the importance of O-acetylation for antibody binding; the lack of binding of protective antibodies to short GXM fragments; the existence of epitopes that elicit non-protective antibodies; and the self-aggregation of GXM chains—indicating that molecular modelling can play a role in the rational design of conjugate vaccines. [ABSTRACT FROM AUTHOR]

Published

2020