Src kinases and not JAKs activate STATs during IL-3 induced myeloid cell proliferation

Chaturvedi, Priya; Reddy, Meera; Reddy, E. Premkumar

doi:10.1038/sj.onc.1201972

Cited by 132 publications

(132 citation statements)

References 27 publications

(48 reference statements)

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“…In this study, we found G-CSF-mediated STAT phosphorylation is not Lyn-dependent by means of antisense JAK or AG490 inhibition experiments. Consistent with this, overexpression of dominant-negative JAK2 had no effect on Srcmediated phosphorylation of STATs (Chaturvedi et al, 1998). Combined with our results, this suggests that two independent pathways exist that mediate STAT activation, one dependent on the JAKs and the other dependent on Src kinases.…”

Section: Discussionsupporting

confidence: 90%

Engagement of the B-cell antigen receptor activates STAT through Lyn in a Jak-independent pathway

2006

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Engagement of the B-cell antigen receptor (BCR) initiated by the Src kinase Lyn triggers rapid signaling cascades, leading to proliferation, differentiation or growth arrest of B cells. The Janus kinase (JAK)-STAT (signal transducer and activator of transcription) pathway, activated through cytokine receptors, mediates similar responses. Hypothesizing that Src and JAK pathways engage in crosstalk in B-cell signaling, we studied wild-type and Lyn-null B-cell lines, which express BCR. We found that activated BCR results in tyrosine phosphorylation of JAK-STAT, which required Lyn. To confirm that STAT activation is not due to JAK, we cloned the chicken homologs of JAK1 and JAK2 and made their antisense constructs. In cells expressing antisense JAK1 and JAK2, tyrosine phosphorylation of STAT was not inhibited following BCR stimulation. Using activation loop-specific phosphotyrosine antibodies, we did not detect phospho-JAK1 and phospho-JAK2 after BCR stimulation. The JAK inhibitor AG490 did not inhibit the tyrosine phosphorylation of Lyn or STAT after BCR simulation. An in vitro phosphorylation assay showed that Lyn directly phosphorylates STAT3. In an electrophoretic mobility shift assay, BCR stimulation led to enhanced DNA binding of the STAT3 in DT40, but not in the Lynnull cells. We conclude that BCR engagement activates the STAT pathway via Lyn, independent of JAK.

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Section: Discussionsupporting

confidence: 90%

Engagement of the B-cell antigen receptor activates STAT through Lyn in a Jak-independent pathway

2006

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“…Several groups have reported that v-src and Src-kinase can activate STAT3 (Cao et al, 1996;Campbell et al, 1997;Chaturvedi et al, 1998). In addition, Marrero et al (1995) reported that activation of STAT3 can be induced or enhanced by GCRs, in particular by angiotensin II AT 1 receptor.…”

Section: Resultsmentioning

confidence: 99%

“…As STAT3 has been shown to regulate mitogenesis or/and prevention of cell apoptosis in various cell types (Fukada et al, 1996;Chaturvedi et al, 1998) and 85 kDa STAT3D proteins are overexpressed in a i2 -G204A and a i2 -G204A/v-fms cells, we investigated whether excessive STAT3D expression inhibits NIH3T3 cell proliferation. Cells stably transfected with STAT3D55C cDNA showed increased expression of 85 kDa STAT3D (Figure 8), but also, as observed previously (Kim and Baumann, 1997), a slightly decreased expression of 89 kDa STAT3.…”

Section: Resultsmentioning

confidence: 99%

“…The regulation of Src-kinase activity by G i2 proteins is speci®c: Fyn expression and activity were not altered in cells expressing a i2 -G204A, indicating that Fyn did not compensate for Src in signalling leading to cell proliferation. Indeed, the role played by Src in the regulation of cell proliferation is thought to be essential: it was reported that Src stimulates JAK1 and STAT3 (Cao et al, 1996 ;Campbell et al, 1997;Chaturvedi et al, 1998) and also that impaired ®broblast proliferation related to de®cient Src-kinase activity could be rescued by c-myc (Roche et al, 1995b). In our model, we found no evidence linking Src activity and c-myc expression; v-fms expression increased c-myc levels to similar levels in cells with active or inactive G i2 proteins (i.e., intact or de®cient Src-kinase activity).…”

Section: Discussionmentioning

confidence: 99%

“…STAT3 is activated by phosphorylation on tyrosine residues by a number of cytokines (including IL-3, IL-6, CSF-1) and STAT3 activation by IL-3 or IL-6 requires Src-kinase (Chaturvedi et al, 1998;Wang et al, 1999). Similarly, we found that v-fms induces constitutive tyrosine phosphorylation of STAT3 in cells with active G i2 and Src proteins, but not in cells with de®cient G i2 and/or Src proteins, indicating that v-fms requires Src to activate STAT3 and that Src-mediated activation of STAT3 may be the decisive event regulated by G i2 proteins in the transduction of CSF-1R signalling.…”

Section: Discussionmentioning

confidence: 99%

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Regulation by Gi2 proteins of v-fms-induced proliferation and transformation via Src-kinase and STAT3

1999

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We previously showed that G i2 proteins interfere with the transduction of CSF-1 receptor (CSF-1R) proliferation signals (Corre and Hermouet, 1995). To identify CSF-1R pathways controlled by G i2 , we transfected v-fms, the oncogenic equivalent of CSF-1R, in NIH3T3 cells in which G i2 proteins were inactivated by stably expressing a dominant negative mutant form of the a subunit of G i2 (a i2 -G204A). Expression of a i2 -G204A resulted in decreased Src-kinase activity, delayed activation of p42 ERK-MAPK, decreased cyclin D1 expression and reduced proliferation in response to serum. In a i2 -G204A cells transfected with v-fms, Src-kinase activity remained de®cient but p42 MAPK activity and cyclin D1 expression were similar to those of vector/v-fms cells, suggesting that v-fms bypasses Src to activate the ERK-MAPK cascade. However, DNA synthesis and focus formation were inhibited by up to 80% in a i2 -G204A/vfms cells compared to vector/v-fms cells. We found that tyrosine phosphorylation of STAT3, also activated by CSF-1R/v-fms, was inhibited in a i2 -G204A/v-fms cells; in addition, expression of an 85 kDa, C-terminal truncated form of STAT3 (STAT3D) was constitutively increased. Both the inhibition of v-fms-induced STAT3 tyrosine phosphorylation and the increased expression of STAT3D were reproduced by transfecting a dominant negative mutant of Src. Last, we show that expression of STAT3D55C, a mutant form of STAT3 lacking the last 55 C-terminal amino acids, is su cient to inhibit DNA synthesis and v-fms-induced transformation in NIH3T3 cells. In summary, adequate regulation by G i2 proteins of the activity of both Src-kinase and STAT3 is required for optimal cell proliferation in response to CSF-1R/vfms.

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Oncogenes, Oncoproteins

Baker¹,

Reddy²

2002

Encyclopedia of Molecular Biology

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Src kinases and not JAKs activate STATs during IL-3 induced myeloid cell proliferation

Cited by 132 publications

References 27 publications

Engagement of the B-cell antigen receptor activates STAT through Lyn in a Jak-independent pathway

Engagement of the B-cell antigen receptor activates STAT through Lyn in a Jak-independent pathway

Regulation by Gi2 proteins of v-fms-induced proliferation and transformation via Src-kinase and STAT3

Oncogenes, Oncoproteins

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