PITSLRE protein kinase activity is associated with apoptosis

Lahti, Jill M.; Xiang, Jialing; Heath, Lucie S.; Campana, Dario; Kidd, Vincent J.

doi:10.1128/mcb.15.1.1

Cited by 204 publications

(169 citation statements)

References 61 publications

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“…Activation of cyclin dependent-protein kinase (CDK), Cdc2 kinase was correlated with apoptosis of lymphoma cells induced by granzyme B (Shi et al, 1994). An additional CDK, p58 PITSRLE induced apoptosis upon overexpression in Chinese hamster ovary cells and was activated by Fas-stimulation (Lahti et al, 1995). FAST and RICK (also known as RIP2) kinases are also implicated in Fas-mediated apoptosis (Tian et al, 1995;Inohara et al, 1998;McCarthy et al, 1998).…”

Section: Introductionmentioning

confidence: 99%

Death-associated protein kinase 2 is a new calcium/calmodulin-dependent protein kinase that signals apoptosis through its catalytic activity

et al. 1999

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We have identi®ed and characterized a new calcium/ calmodulin (Ca 2+ /CaM) dependent protein kinase termed death-associated protein kinase 2 (DAPK2) that contains an N-terminal protein kinase domain followed by a conserved CaM-binding domain with signi®cant homologies to those of DAP kinase, a protein kinase involved in apoptosis. DAPK2 mRNA is expressed abundantly in heart, lung and skeletal muscle. The mapping results indicated that DAPK2 is located in the central region of mouse chromosome 9. In vitro kinase assay revealed that DAPK2 is autophosphorylated and phosphorylates myosin light chain (MLC) as an exogenous substrate. DAPK2 binds directly to CaM and is activated in a Ca 2+ /CaM-dependent manner. A constitutively active DAPK2 mutant is generated by removal of the CaMbinding domain (DCaM). Treatment of agonists that elevate intracellular Ca 2+ -concentration led to the activation of DAPK2 and transfection studies revealed that DAPK2 is localized in the cytoplasm. Overexpression of DAPK2, but not the kinase negative mutant, signi®cantly induced the morphological changes characteristic of apoptosis. These results indicate that DAPK2 is an additional member of DAP kinase family involved in apoptotic signaling.

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Section: Introductionmentioning

confidence: 99%

Death-associated protein kinase 2 is a new calcium/calmodulin-dependent protein kinase that signals apoptosis through its catalytic activity

et al. 1999

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“…As observed with Myc, elevated cyclin levels can result either in transformation (Motokura et al, 1991;Withers et al, 1991) or in apoptosis (Freeman et al, 1994;Hoang et al, 1994;Lahti et al, 1995;Meikrantz et al, 1994;Meikrantz and Schlegel, 1996;Sherr and Roberts, 1995;Shi et al, 1994), and dominant negative mutants of cdc2, cdk2 and cdk3 can suppress apoptosis (Meikrantz and Schlegel, 1996). Direct links between the activation of Myc and cdks have been proposed (Galaktionov et al, 1996;Hoang et al, 1994;Rudolph et al, 1996;Steiner et al, 1995) and build on the concept that the inappropriate overexpression of c-myc may cause aberrant cell cycle events as a prelude to apoptosis in cells predisposed to this condition.…”

Section: Introductionmentioning

confidence: 99%

Quiescence versus apoptosis: Myc abundance determines pathway of exit from the cell cycle

et al. 1998

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“…Interestingly, 1p22 band contains the dihydropyrimidine dehydrogenase gene, which encodes an initial and rate-limiting enzyme acting in the uracil and thymine catabolic pathways and being responsible for degradation of 5-fluorouracil, which is also considered as a potential prognostic marker for breast cancers (Li et al 2004). Moreover, 1p33 band contains the cyclin-dependent kinase inhibitor 2C gene encoding p18 of the INK4 family which functions as a cell cycle regulator that controls G 1 progression via inhibition of CDK4 (Guan et al 1994), whereas the cell division cycle 2-like 2 (PITSLRE protein) variant 3 gene, encoding a member of the subfamily of p34 cdc2 -related protein kinases which intervene in the regulation of apoptosis, and at least other three potential tumor suppressor genes (i.e., Heir-1, TNFR , and DAN) are located in band 1p36 which contains another aphidicolin-inducible chromosomal fragile site (Lahti et al 1995;Thompson et al 1997;Tunca et al 2000).…”

Section: Discussionmentioning

confidence: 99%

Cytogenetic characterization of HB2 epithelial cells from the human breast

Caradonna

Luparello

2013

In Vitro Cell.Dev.Biol.-Animal

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HB2 is a cell line originated by subcloning of MTSV1-7 mammary luminal epithelial cells isolated from human milk and immortalization via introduction of the gene encoding simian virus 40 (SV40) large T antigen. Despite its wide utilization as non-neoplastic counterpart in assays aimed to elucidating various biochemical and genetical aspects of normal and tumoral breast cells, to our knowledge no literature data have so far appeared concerning the chromosomal characterization of the HB2 cells. Here, we report the cytogenetic characterization of the karyotype of HB2 cells, which puts in evidence the occurrence of changes in chromosomal number and structure and the presence of unidentified chromosomal markers in variable amount. Our results do not detract from the utility of HB2 cells in illustrating fundamental aspects of breast cell biology, but rather interject a note of caution into generalizing results obtained with this cell line to other non-immortalized epithelial cell populations from the human breast. Therefore, this work represents a useful resource for all who want to perform appropriate and focused future studies on this cell line and proposes precise indications for a knowledgeable use of HB2 cells.

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PITSLRE protein kinase activity is associated with apoptosis

Cited by 204 publications

References 61 publications

Death-associated protein kinase 2 is a new calcium/calmodulin-dependent protein kinase that signals apoptosis through its catalytic activity

Death-associated protein kinase 2 is a new calcium/calmodulin-dependent protein kinase that signals apoptosis through its catalytic activity

Quiescence versus apoptosis: Myc abundance determines pathway of exit from the cell cycle

Cytogenetic characterization of HB2 epithelial cells from the human breast

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