Basement membrane remodeling is essential for
            <i>Drosophila</i>
            disc eversion and tumor invasion

Srivastava, Ajay; Pastor-Pareja, José Carlos; Igaki, Tatsushi; Pagliarini, Raymond; Xu, Tian

doi:10.1073/pnas.0611666104

Cited by 182 publications

(245 citation statements)

References 45 publications

(53 reference statements)

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“…The effect of JNK on invasion has been shown to be due to upregulation of targets important in cell migration, such as Paxillin, and in breakdown of the extracellular matrix, such as MMP1 (Beaucher et al 2006;Uhlirova and Bohmann 2006;Srivastava et al 2007;Leong et al 2009), but how JNK blocks differentiation and pupation is currently unknown. Expression of bsk DN also reduced tumor overgrowth to a level commensurate with Ras ACT alone for all except Rac1 1 Ras ACT .…”

Section: Discussionmentioning

confidence: 99%

Identification of Novel Ras-Cooperating Oncogenes in Drosophila melanogaster: A RhoGEF/Rho-Family/JNK Pathway Is a Central Driver of Tumorigenesis

et al. 2011

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We have shown previously that mutations in the apico-basal cell polarity regulators cooperate with oncogenic Ras (Ras ACT ) to promote tumorigenesis in Drosophila melanogaster and mammalian cells. To identify novel genes that cooperate with Ras ACT in tumorigenesis, we carried out a genome-wide screen for genes that when overexpressed throughout the developing Drosophila eye enhance Ras ACT -driven hyperplasia. Ras ACT -cooperating genes identified were Rac1 Rho1, RhoGEF2, pbl, rib, and east, which encode cell morphology regulators. In a clonal setting, which reveals genes conferring a competitive advantage over wildtype cells, only Rac1, an activated allele of Rho1 (Rho1 ACT ), RhoGEF2, and pbl cooperated with Ras ACT , resulting in reduced differentiation and large invasive tumors. Expression of RhoGEF2 or Rac1 with Ras ACT upregulated Jun kinase ( JNK) activity, and JNK upregulation was essential for cooperation. However, in the whole-tissue system, upregulation of JNK alone was not sufficient for cooperation with Ras ACT , while in the clonal setting, JNK upregulation was sufficient for Ras ACT -mediated tumorigenesis. JNK upregulation was also sufficient to confer invasive growth of Ras V12 -expressing mammalian MCF10A breast epithelial cells. Consistent with this, HER2 1 human breast cancers (where human epidermal growth factor 2 is overexpressed and Ras signaling upregulated) show a significant correlation with a signature representing JNK pathway activation. Moreover, our genetic analysis in Drosophila revealed that Rho1 and Rac are important for the cooperation of RhoGEF2 or Pbl overexpression and of mutants in polarity regulators, Dlg and aPKC, with Ras ACT in the whole-tissue context. Collectively our analysis reveals the importance of the RhoGEF/ Rho-family/JNK pathway in cooperative tumorigenesis with Ras ACT .

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Section: Discussionmentioning

confidence: 99%

Identification of Novel Ras-Cooperating Oncogenes in Drosophila melanogaster: A RhoGEF/Rho-Family/JNK Pathway Is a Central Driver of Tumorigenesis

et al. 2011

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“…While Wg is an absolute requirement for CIN-induced tissue overgrowth, 10 MMPs are well-known to contribute to BM degradation both in flies and mammals. [24][25][26] We thus monitored the expression of these 2 JNK targets in tissues depleted of CENP-E or Nsl1. In wild-type wing primordia, Wg is expressed in a stripe that corresponds to the future wing margin (Fig.…”

Section: Ap-gal4uas-myrt/+; Uas-p35/+ (A) Ap-gal4uas-myrt/+; Uas-cmentioning

confidence: 99%

Tumor suppressor roles of CENP-E and Nsl1 inDrosophilaepithelial tissues

2014

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“…In this context, JNK signaling directs growth and invasion instead of promoting cell death. 39,[53][54][55][56] Importantly, Ras can cooperate with other oncogenic pathways that result in JNK activation without directly regulating cell polarity, such as Src 50 and Rho-family GTPases. 57 Remarkably, because JNK activation propagates across imaginal disc epithelia, the cooperation between JNK and Ras does not need to be cell autonomous.…”

Section: Discussionmentioning

confidence: 99%

“…37 Many aspects of human tumorogenesis are recapitulated in mutants of a class of Tumor Suppressor Genes (TSGs) coding for proteins involved in the establishment of apical-basal polarity of epithelial cells. 38,39 These Drosophila tumor models display a loss of cellular architecture, dramatic over-proliferation, basal membrane (BM) degradation and invasive capacity. 39,40 In this context Pastor-Pareja and coworkers investigated the role of the cellular immune system in cancer detection and surveillance and found hemocytes adhered to the tumor surface at the site of BM disruption.…”

Section: Hemocytes and Tumorigenesismentioning

confidence: 99%

“…38,39 These Drosophila tumor models display a loss of cellular architecture, dramatic over-proliferation, basal membrane (BM) degradation and invasive capacity. 39,40 In this context Pastor-Pareja and coworkers investigated the role of the cellular immune system in cancer detection and surveillance and found hemocytes adhered to the tumor surface at the site of BM disruption. 41 In tumor-bearing flies, the increase in hemocyte number-as a consequence of secretion of JAK-STAT activating cytokines by the tumor cells-was suggested to be the means to restrict tumor growth.…”

Section: Hemocytes and Tumorigenesismentioning

confidence: 99%

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