Granulysin Delivered by Cytotoxic Cells Damages Endoplasmic Reticulum and Activates Caspase-7 in Target Cells

Saini, Reena V.; Wilson, C. M.; Finn, Michael W.; Wang, Tianhong; Krensky, Alan M.; Clayberger, Carol

doi:10.4049/jimmunol.1003409

Cited by 63 publications

(64 citation statements)

References 43 publications

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“…These are not mutually exclusive possibilities. Interestingly there is indirect evidence that granulysin, a component of the CL granule, is delivered by perforin into target cells (54). This is consistent with data presented here as granulysin is known to be cationic (55).…”

Section: Discussionsupporting

confidence: 81%

The Perforin Pore Facilitates the Delivery of Cationic Cargos

Stewart

Kondos

Matthews

et al. 2014

Journal of Biological Chemistry

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Background: Perforin is a pore-forming protein that delivers granzymes to eliminate compromised cells. Results:The perforin pore preferentially delivers cationic molecules in comparison to anionic or neutrally charged cargo, which are inefficiently delivered. Conclusion: Perforin delivers cationic cargos more efficiently than anionic or neutral cargos. Significance: This is the first report of charge-based discrimination by the perforin pore.

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Section: Discussionsupporting

confidence: 81%

The Perforin Pore Facilitates the Delivery of Cationic Cargos

Stewart

Kondos

Matthews

et al. 2014

Journal of Biological Chemistry

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“…Granulysin is known for its direct lytic effect on a wide variety of pathogens (36,37), its role in apoptosis (38,39), and its alarmin-like function (40). Granzyme B, a serine protease, is associated with granulysin in some of these functions, particularly in the induction of apoptosis.…”

Section: Discussionmentioning

confidence: 99%

Granule Exocytosis of Granulysin and Granzyme B as a Potential Key Mechanism in Vaccine-Induced Immunity in Cattle against the Nematode Ostertagia ostertagi

et al. 2013

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dOstertagia ostertagi is considered one of the most economically important bovine parasites. As an alternative to anthelmintic treatment, an experimental host-protective vaccine was previously developed on the basis of ASP proteins derived from adult worms. Intramuscular injection of this vaccine, combined with QuilA as an adjuvant, significantly reduced fecal egg counts by 59%. However, the immunological mechanisms triggered by the vaccine are still unclear. Therefore, in this study, the differences in immune responses at the site of infection, i.e., the abomasal mucosa, between ASP-QuilA-vaccinated animals and QuilA-vaccinated control animals were investigated on a transcriptomic level by using a whole-genome bovine microarray combined with histological analysis. Sixty-nine genes were significantly impacted in animals protected by the vaccine, 48 of which were upregulated. A correlation study between the parasitological parameters and gene transcription levels showed that the transcription levels of two of the upregulated genes, those for granulysin (GNLY) and granzyme B (GZMB), were negatively correlated with cumulative fecal egg counts and total worm counts, respectively. Both genes were also positively correlated with each other and with another upregulated gene, that for the IgE receptor subunit (FCER1A). Surprisingly, these three genes were also correlated significantly with CMA1, which encodes a mast cell marker, and with counts of mast cells and cells previously described as globule leukocytes. Furthermore, immunohistochemical data showed that GNLY was present in the granules of globule leukocytes and that it was secreted in mucus. Overall, the results suggest a potential role for granule exocytosis by globule leukocytes, potentially IgE mediated, in vaccine-induced protection against O. ostertagi.

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“…It is released from effector cells by exocytosis in preformed granules, in proximity to target cells (Saini et al, 2011). NK cells spontaneously release GNLY within 2 h, while T cells need three to five days for GNLY release after their activation .…”

Section: Introductionmentioning

confidence: 99%