Role of Jun N-terminal Kinase (JNK) signaling in the wound healing and regeneration of a Drosophila melanogaster wing imaginal disc

Mattila, Jaakko; Omelyanchuk, L. V.; Kyttala, Satu; Turunen, Heikki; Nokkala, Seppo

doi:10.1387/ijdb.052006jm

Cited by 89 publications

(100 citation statements)

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“…Other stocks used were: dlg-RNAi 4689 C2V (gift from B. Dickson, Dietzl et al 2007), validated for knockdown of Dlg and specificity , msn 06946 (msn-lacZ) (Mattila et al 2005); UAS-P35 (Hay et al 1994); UAS-bsk K53R (UAS-bsk DN ) (Weber et al 2000), UAS-aPKC DN (Betschinger et al 2003); UAS-aPKC CAAX-DN (Sotillos et al 2004); UASRas85D V12 (UAS-Ras ACT ) (Karim and Rubin 1998); UASRac1 N17 (UAS-Rac1 DN ) (Luo et al 1994); UAS-Rho1 RNAi #12734 [Vienna Drosophila Resource Center (VDRC), Dietzl et al 2007] and scrib 1 (D. Bilder).…”

Section: Methodsmentioning

confidence: 99%

“…To determine the involvement of JNK signaling in the cooperation of ey.Ras ACT with RhoGEF2 and Rac1, we first tested whether JNK activity was increased in these eye discs, using the msn-lacZ reporter to monitor JNK pathway activity (Mattila et al 2005). Expression of Ras ACT via ey-GAL4 resulted in a weak induction of msn-lacZ in some cells in the eye disc ( Figure 3, A and B), which was expected because of previous findings on the regulation of Jun and Fos activity via the Ras-MAPK signaling pathway (Kockel et al 1997;Ciapponi et al 2001).…”

Section: Uas-pbl-gfp#8mentioning

confidence: 99%

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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: Methodsmentioning

confidence: 99%

Section: Uas-pbl-gfp#8mentioning

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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“…Recently, Wagner and co-workers provided evidence that neoblasts, which are adult pluripotent stem cells, underlie the remarkable regenerative abilities of planarians (Wagner et al, 2011 Table 1 in Stocum and Zupanc, 2008). Although different, all these processes share signaling pathways and molecular mechanisms to restore normal function of the affected tissue (Bosch et al, 2005;Mattila et al, 2005;Gurtner et al, 2008). Determining how common signaling pathways are used in different processes is one of the main questions in developmental biology and regenerative medicine.…”

Section: Regeneration: Blastema Formation and The Role Of Adult Stem mentioning

confidence: 99%

“…It appears that the JNK pathway is activated in a gradient emanating from the wound limited by the scab and diffuses to the syncytium to promote cell spreading and reepithelialization. It has also been shown that the JNK pathway and its upstream regulators, the Rho family of small GTPases, are involved in localization of Nonmuscle Myo II to larval wounds (Rä met et al, 2002;Jacinto et al, 2002;Galko and Krasnow, 2004;Mattila et al, 2005;Baek et al, 2010;Kwon et al, 2010). The JNK pathway and Fos activate the expression of MMP-1, which degrades matricellular proteins during wound healing, as well as during disc eversion/regeneration and tumor invasion in Drosophila (Uhlirova and Bohmann, 2006;Srivastava et al, 2007;McClure et al, 2008).…”

Section: Wounding Drosophila Embryos Larvae and Adultsmentioning

confidence: 99%

Drosophila as a model of wound healing and tissue regeneration in vertebrates

Belacortu

Paricio

2011

Developmental Dynamics

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Understanding the molecular basis of wound healing and regeneration in vertebrates is one of the main challenges in biology and medicine. This understanding will lead to medical advances allowing accelerated tissue repair after wounding, rebuilding new tissues/organs and restoring homeostasis. Drosophila has emerged as a valuable model for studying these processes because the genetic networks and cytoskeletal machinery involved in epithelial movements occurring during embryonic dorsal closure, larval imaginal disc fusion/regeneration, and epithelial repair are similar to those acting during wound healing and regeneration in vertebrates. Recent studies have also focused on the use of Drosophila adult stem cells to maintain tissue homeostasis. Here, we review how Drosophila has contributed to our understanding of these processes, primarily through live-imaging and genetic tools that are impractical in mammals. Furthermore, we highlight future research areas where this insect may provide novel insights and potential therapeutic strategies for wound healing and regeneration. Developmental Dynamics 240:2379-2404,

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“…22 In this period of non-responsiveness to wound signals embryonic tissues can still repair and they do so generally without producing scarring or fibrosis, suggesting the intriguing idea that scars are the result of the inflammatory process that takes place at the adults wounds. 25 Beyond their roles in the embryo, Drosophila hemocytes play an important role in efficiently fighting infections 26 and repairing tissue damage [27][28][29] during the larval and adult stages of the fly. Just before hatching into larva, the heart (dorsal vessel) begins to beat, and the hemolymph (fly blood) circulation is established.…”

Section: Hemocytes and Tumorigenesismentioning

confidence: 99%