2001
DOI: 10.1002/1529-0131(200111)44:11<2642::aid-art444>3.0.co;2-8
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Secondary necrosis is a source of proteolytically modified forms of specific intracellular autoantigens: Implications for systemic autoimmunity

Abstract: Objective Specific autoantigens targeted in systemic autoimmunity undergo posttranslational modifications, such as cleavage, during cell death that could potentially enhance their immunogenicity. In light of the increasing interest in the immunologic consequences of defective clearance of apoptotic cells, we sought to determine whether autoantigens cleaved during apoptosis undergo an additional wave of proteolysis as apoptosis progresses to secondary necrosis in the absence of phagocytosis. Methods Apoptosis w… Show more

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Cited by 103 publications
(108 citation statements)
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“…In the case of Topo I, a signature necrotic fragment of 45 kDa was detected, consistent with previous reports demonstrating that the generation of this fragment is a distinctive feature of necrotic cell death. 42,43 The pattern of Figure 3 Transfected HA-E6 retains biological activity in both sensitive and resistant clones. (a) ELISA measurement of baseline and induced levels of p53 in E6-expressing clones.…”
Section: Expression Of E6 Results In a Loss Of Cellular P53mentioning
confidence: 99%
“…In the case of Topo I, a signature necrotic fragment of 45 kDa was detected, consistent with previous reports demonstrating that the generation of this fragment is a distinctive feature of necrotic cell death. 42,43 The pattern of Figure 3 Transfected HA-E6 retains biological activity in both sensitive and resistant clones. (a) ELISA measurement of baseline and induced levels of p53 in E6-expressing clones.…”
Section: Expression Of E6 Results In a Loss Of Cellular P53mentioning
confidence: 99%
“…A disturbed clearance of apoptotic cells, as has been observed in some patients with SLE, facilitates the release of heat-shock proteins (33), nucleosomes (34), calreticulin (35,36), and other intracellular contents. In addition, modifications of these autoantigens during programmed cell death can render them more immunogenic (34,37,38). It has also been shown that in mice genetically predisposed to autoimmune disease, bacterial DNA can elicit anti-DNA autoantibodies under conditions in which mammalian DNA is inactive (39).…”
Section: Discussionmentioning
confidence: 99%
“…In some experiments, cells were pretreated with the cathepsin L inhibitor Z-FY-CHO (150 M) or with individual caspase inhibitors 1 hour prior to addition of TNF␣. Quantification of cytoplasmic membrane rupture, indicative of necrosis, was performed by trypan blue exclusion (11). Morphologic analysis of cells was performed using an Olympus IX70 inverted microscope (Olympus, Melville, NY) equipped with Hoffman modulation contrast.…”
Section: Methodsmentioning
confidence: 99%
“…Topo I fragments of 72-75 kd are also produced by granzyme B both in vitro and during cell death induced by cytotoxic T lymphocytes (14). Our group demonstrated previously that topo I is also cleaved into fragments of approximately 70 kd and 45 kd in cells undergoing primary or secondary necrosis (10,11).…”
mentioning
confidence: 92%
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