2007
DOI: 10.1101/gad.1480007
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Bcl2L12 inhibits post-mitochondrial apoptosis signaling in glioblastoma

Abstract: Glioblastoma (GBM) is an astrocytic brain tumor characterized by an aggressive clinical course and intense resistance to all therapeutic modalities. Here, we report the identification and functional characterization of Bcl2L12 (Bcl2-like-12) that is robustly expressed in nearly all human primary GBMs examined. Enforced Bcl2L12 expression confers marked apoptosis resistance in primary cortical astrocytes, and, conversely, its RNA interference (RNAi)-mediated knockdown sensitizes human glioma cell lines toward a… Show more

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Cited by 148 publications
(176 citation statements)
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“…1, left), while other heat shock proteins, caspases, and their (post-mitochondrial) inhibitors, such as members of the IAP family, are not differentially expressed. 6,17 In addition, primary human GBM tumor specimens revealed striking co-expression of Bcl2L12 and αB-crystallin, and Bcl2L12-driven (U87MG) xenografts showed significant upregulation of αB-crystallin, confirming a Bcl2L12-aB-crystallin signaling axis axis not only in glial cells in vitro, but also in GBM tumors in vivo. 17 The induction of αB-crystallin expression by Bcl2L12 appears to be highly relevant.…”
Section: αB-crystallin Is a Novel Gliomagenic Oncoproteinmentioning
confidence: 79%
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“…1, left), while other heat shock proteins, caspases, and their (post-mitochondrial) inhibitors, such as members of the IAP family, are not differentially expressed. 6,17 In addition, primary human GBM tumor specimens revealed striking co-expression of Bcl2L12 and αB-crystallin, and Bcl2L12-driven (U87MG) xenografts showed significant upregulation of αB-crystallin, confirming a Bcl2L12-aB-crystallin signaling axis axis not only in glial cells in vitro, but also in GBM tumors in vivo. 17 The induction of αB-crystallin expression by Bcl2L12 appears to be highly relevant.…”
Section: αB-crystallin Is a Novel Gliomagenic Oncoproteinmentioning
confidence: 79%
“…4,5 Detailed mRNA expression analyses and cell-culture based oncogene cooperation assays of genes within this chromosomal region pointed to Bcl2L12 as a putative oncoprotein based on its frequent mRNA upregulation in GBM and significant in vitro transforming activity. 6 Immunohistochemical tissue microarray (IHC-TMA) analysis confirmed robust Bcl2L12 expression in nearly all primary GBM with low or absent expression in lower-grade astrocytoma and normal brain tissue. 6 This robust expression profile in GBM prompted a multi-level functional characterization of Bcl2L12 to assess its impact on glioma-relevant signaling pathways.…”
Section: Bcl2l12 Is a Structurally Distinctive Member Of The Bcl-2 Famentioning
confidence: 98%
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