Murine Hyperglycemic Vasculopathy and Cardiomyopathy: Whole-Genome Gene Expression Analysis Predicts Cellular Targets and Regulatory Networks Influenced by Mannose Binding Lectin

Zou, Congming; Bonte, Laura R. La; Pavlov, Vasile I.; Stahl, Gregory L.

doi:10.3389/fimmu.2012.00015

Cited by 6 publications

(3 citation statements)

References 51 publications

(71 reference statements)

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“…In this context, treatment of C. neoformans with WGA could interfere with polysaccharide synthesis, promoting a general attenuation in GXM metabolism, or simply block polysaccharide secretion. It has been described that binding of lectins to the surface of eukaryotic cells can profoundly modify intracellular signaling cascades and regulate gene expression (O’Brien et al, 2012; Zou et al, 2012). In fact, we observed that WGA caused an effective ablation of transcription levels of eight genes directly or indirectly involved in capsule formation and a discrete attenuation in the transcription of the gene encoding the subunit α of protein G, an important mediator of signaling pathways in C. neoformans (Alspaugh et al, 1997; D’Souza et al, 2001).…”

Section: Discussionmentioning

confidence: 99%

Binding of the wheat germ lectin to Cryptococcus neoformans chitooligomers affects multiple mechanisms required for fungal pathogenesis

Fonseca

Guimarães

Kmetzsch

et al. 2013

Fungal Genetics and Biology

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The principal capsular component of Cryptococcus neoformans, glucuronoxylomannan (GXM), interacts with surface glycans, including chitin-like oligomers. Although the role of GXM in cryptococcal infection has been well explored, there is no information on how chitooligomers affect fungal pathogenesis. In this study, surface chitooligomers of C. neoformans were blocked through the use of the wheat germ lectin (WGA) and the effects on animal pathogenesis, interaction with host cells, fungal growth and capsule formation were analyzed. Treatment of C. neoformans cells with WGA followed by infection of mice delayed mortality relative to animals infected with untreated fungal cells. This observation was associated with reduced brain colonization by lectin-treated cryptococci. Blocking chitooligomers also rendered yeast cells less efficient in their ability to associate with phagocytes. WGA did not affect fungal viability, but inhibited GXM release to the extracellular space and capsule formation. In WGA-treated yeast cells, genes that are involved in capsule formation and GXM traffic had their transcription levels decreased in comparison with untreated cells. Our results suggest that cellular pathways required for capsule formation and pathogenic mechanisms are affected by blocking chitin-derived structures at the cell surface of C. neoformans. Targeting chitooligomers with specific ligands may reveal new therapeutic alternatives to control cryptococcosis.

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Section: Discussionmentioning

confidence: 99%

Binding of the wheat germ lectin to Cryptococcus neoformans chitooligomers affects multiple mechanisms required for fungal pathogenesis

Fonseca

Guimarães

Kmetzsch

et al. 2013

Fungal Genetics and Biology

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“…Use of such methods were employed in a hyperglycemia model to study acute vasculopathy, cardiomyopathy, the specific role of MBL (Zou et al, 2012) and other complement components (Stahl laboratory; unpublished data) compared to WT. Knowledge derived from these data sets will allow us to formulate gene interaction sets for therapeutic targeting and hypothesis testing (Zou et al, 2012). …”

Section: Complement I/r Injuries In the Era Of –Omics Researchmentioning

confidence: 99%

The complement system in ischemia–reperfusion injuries

et al. 2012

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Tissue injury and inflammation following ischemia and reperfusion of various organs has been recognized for many years. Many reviews have been written over the last several decades outlining the role of complement in ischemia/reperfusion injury. This short review provides a current state of the art knowledge on the complement pathways activated, complement components involved and a review of the clinical biologics/inhibitors used in the clinical setting of ischemia/reperfusion. This is not a complete review of the complement system in ischemia and reperfusion injury but will give the reader an updated view point of the field, potential clinical use of complement inhibitors, and the future studies needed to advance the field.

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“…The oxido-reductive signalling plays integral roles in vascular remodelling processes, importantly in the regulation of cytoskeletal dynamics and modulation of smooth muscle cell differentiation2770. Concomitant identification of actin-related complexes and tubulins in the Huntington disease pathway in the current exploratory study comes as no surprise as these are arguably among the most overwhelmingly expressed proteins in cells, which assemble to construct complex networks of cytoskeleton7172, and this is in agreement with the significant detection of the actin-cytoskeleton processes in the porcine sPCA (Fig. 4).…”

Section: Discussionmentioning

confidence: 80%

First insight into the proteome landscape of the porcine short posterior ciliary arteries: Key signalling pathways maintaining physiologic functions

Manicam

Perumal

Pfeiffer

et al. 2016

Sci Rep

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Short posterior ciliary arteries (sPCA) provide the major blood supply to the optic nerve head. Emerging evidence has linked structural and functional anomalies of sPCA to the pathogenesis of several ocular disorders that cause varying degrees of visual loss, particularly anterior ischaemic optic neuropathy and glaucoma. Although the functional relevance of this vascular bed is well-recognized, the proteome of sPCA remains uncharacterized. Since the porcine ocular system closely resembles that of the human’s and is increasingly employed in translational ophthalmic research, this study characterized the proteome of porcine sPCA employing the mass spectrometry-based proteomics strategy. A total of 1742 proteins and 10527 peptides were identified in the porcine sPCA. The major biological processes involved in the maintenance of physiological functions of the sPCA included redox and metabolic processes, and cytoskeleton organization. These proteins were further clustered into diverse signalling pathways that regulate vasoactivity of sPCA, namely the tight junction, α- and β-adrenoceptor, 14-3-3, nitric oxide synthase and endothelin-1 -mediated signalling pathways. This study provides the first insight into the complex mechanisms dictating the vast protein repertoire in normal vascular physiology of the porcine sPCA. It is envisioned that our findings will serve as important benchmarks for future studies of sPCA.

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Murine Hyperglycemic Vasculopathy and Cardiomyopathy: Whole-Genome Gene Expression Analysis Predicts Cellular Targets and Regulatory Networks Influenced by Mannose Binding Lectin

Cited by 6 publications

References 51 publications

Binding of the wheat germ lectin to Cryptococcus neoformans chitooligomers affects multiple mechanisms required for fungal pathogenesis

Binding of the wheat germ lectin to Cryptococcus neoformans chitooligomers affects multiple mechanisms required for fungal pathogenesis

The complement system in ischemia–reperfusion injuries

First insight into the proteome landscape of the porcine short posterior ciliary arteries: Key signalling pathways maintaining physiologic functions

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