Granzymes are the essential downstream effector molecules for the control of primary virus infections by cytolytic leukocytes

Müllbacher, Arno; Waring, Paul; Hla, Ron Tha; Tran, Thao; Chin, Seow; Stehlé, Thomas; Museteanu, C; Simon, Markus M.

doi:10.1073/pnas.96.24.13950

Cited by 195 publications

(184 citation statements)

References 47 publications

(56 reference statements)

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“…GzmA À / À and GzmB À / À mice each showed only marginally increased susceptibility to ectromelia in comparison with WT; however, GzmA À / À B À / À mice were highly susceptible, similar to Pfp À / À mice. 29 This demonstrates the importance of different Gzms cooperatively mediating alternative pathways to cell death. Consistent with previous reports showing modest cytotoxic activity for mGzmA, but none for its human counterpart, 10 we found that proteolytically active recombinant human GzmA (hGzmA) was very poorly cytotoxic when administered with Pfp (Supplementary Figure S7).…”

Section: Discussionmentioning

confidence: 93%

Mouse granzyme A induces a novel death with writhing morphology that is mechanistically distinct from granzyme B-induced apoptosis

et al. 2013

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Human and mouse granzyme (Gzm)B both induce target cell apoptosis in concert with pore-forming perforin (Pfp); however the mechanisms by which other Gzms induce non-apoptotic death remain controversial and poorly characterised. We used timelapse microscopy to document, quantitatively and in real time, the death of target cells exposed to primary natural killer (NK) cells from mice deficient in key Gzms. We found that in the vast majority of cases, NK cells from wild-type mice induced classic apoptosis. However, NK cells from syngeneic Gzm B-deficient mice induced a novel form of cell death characterised by slower kinetics and a pronounced, writhing, 'worm-like' morphology. Dying cells initially contracted but did not undergo membrane blebbing, and annexin-V staining was delayed until the onset of secondary necrosis. As it is different from any cell death process previously reported, we tentatively termed this cell death 'athetosis'. Two independent lines of evidence showed this alternate form of death was due to Gzm A: first, cell death was revealed in the absence of Gzm B, but was completely lost when the NK cells were deficient in both Gzm A and B; second, the athetotic morphology was precisely reproduced when recombinant mouse Gzm A was delivered by an otherwise innocuous dose of recombinant Pfp. Gzm A-mediated athetosis did not require caspase activation, early mitochondrial disruption or generation of reactive oxygen species, but did require an intact actin cytoskeleton and was abolished by latrunculin B and mycalolide B. This work defines an authentic role for mouse Gzm A in granule-induced cell death by cytotoxic lymphocytes.

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Section: Discussionmentioning

confidence: 93%

Mouse granzyme A induces a novel death with writhing morphology that is mechanistically distinct from granzyme B-induced apoptosis

et al. 2013

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“…One example being poxvirus-encoded serine protease inhibitors that can severely curtail cytolytic effector functions, most probably by inhibiting Fas-mediated and caspase-facilitated PS exposure, resulting in uncontrolled viral spread. 36 This diversity in effector function of cytolytic pathways will also be to the host's benefit in tumor elimination.…”

Section: Discussionmentioning

confidence: 99%

Granzyme B-induced cell death exerted by ex vivo CTL: discriminating requirements for cell death and some of its signs

et al. 2007

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Granzyme B (gzmB) of cytotoxic T lymphocytes (CTL) is essential for recovery from intracellular pathogens, but the molecular basis of its action is still unresolved. Here, we analyzed gzmB-mediated death pathways under physiological conditions using ex vivo virus-immune CTLs that express perf and gzmB, but not gzmA (gzmB þ CTL). We show that gzmB þ CTL abrogate target cell proliferation most likely by inducing cell death, independent of caspases and mitochondrial signaling. In addition, the data reveal that gzmB þ CTL independently induce pro-apoptotic processes either via caspase-3/-7, leading to plasma membrane perturbance and ROS production or via Bid/Bak/Bax, resulting in cytochrome c release and that both pathways elicit loss of DW m . Our data provide evidence for a pleiotropic pro-apoptotic function of gzmB presumably to counteract evasion strategies of pathogens and to control tumors.

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“…[42][43][44] In vivo, grB À/À knockout mice have shown enhanced susceptibility to mouse cytomegalovirus (MCMV), ectromelia virus, reduced graft versus host disease, and a reduced ability to clear allogeneic tumors. [45][46][47][48] However, in various other models, GrB-deficient mice remain competent at viral and tumor clearance, which is likely a reflection of Gr redundancy in these animals. 49 Granzyme H. GrH was identified through screening cDNA libraries derived from cytotoxic cells.…”

Section: Mechanisms Of Cytotoxicity and Physiological Roles Of Grsmentioning

confidence: 99%

A quarter century of granzymes

2011

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Granzymes are the essential downstream effector molecules for the control of primary virus infections by cytolytic leukocytes

Cited by 195 publications

References 47 publications

Mouse granzyme A induces a novel death with writhing morphology that is mechanistically distinct from granzyme B-induced apoptosis

Mouse granzyme A induces a novel death with writhing morphology that is mechanistically distinct from granzyme B-induced apoptosis

Granzyme B-induced cell death exerted by ex vivo CTL: discriminating requirements for cell death and some of its signs

A quarter century of granzymes

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