An absolute requirement for both the type II and type I receptors, punt and thick veins, for Dpp signaling in vivo

Ruberte, Esther; Marty, Thomas; Nellen, Denise; Affolter, Markus; Basler, Konrad

doi:10.1016/0092-8674(95)90292-9

Cited by 293 publications

(197 citation statements)

References 50 publications

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“…Punt is the type II receptor for Dpp, whereas Thick veins (Tkv) and Saxophone (Sax) are the type I receptors for it (Brummel et al 1994;Nellen et al 1994;Penton et al 1994;Xie et al 1994;Letsou et al 1995;Ruberte et al 1995). Sax also propagates signals of another Drosophila ligand, Screw (Scw) (Neul & Ferguson 1998;Nguyen et al 1998).…”

Section: Introductionmentioning

confidence: 99%

Schnurri interacts with Mad in a Dpp‐dependent manner

et al. 2000

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Background: Decapentaplegic (Dpp) is a member of the transforming growth factor-b superfamily. Dpp governs various developmental processes in Drosophila through the transcriptional regulation of a variety of genes. Signals of Dpp are transmitted from the cell membrane to the nucleus by Medea and Mad, both belonging to the Smad protein family. Mad was shown to bind to the Dpp-responsive element in genes such as vestigial, labial, and Ultrabithorax. The DNA binding af®nity of Smad proteins is relatively low, and requires other nuclear factor(s) to form stable DNA binding complexes. schnurri (shn) was identi®ed as a candidate gene acting downstream of

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Section: Introductionmentioning

confidence: 99%

Schnurri interacts with Mad in a Dpp‐dependent manner

et al. 2000

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“…Mutations in each gene lead to embryos with severe dorsal and anterior open cuticles indicative of a failure of DC and head involution. Loss of JNK pathway activity has (Glise & Noselli, 1997;Harden et al, 1995;1999) (Glise & Noselli, 1997;Harden et al, 1995;1999 (Padgett et al, 1987;Gelbart, 1987) (A olter et al, 1994;Brummel et al, 1994;Nellen et al, 1994;Penton et al, 1994) Ruberte et al, 1995) (Hudson et al, 1998) (Das et al, 1998;Hudson et al, 1998;Wisotzkey et al, 1998) Grieder et al, 1995;Staehling-Hampton et al, 1995) several consequences that contribute to a failure of DC. Mutant embryos exhibit a loss of dpp expression in LE cells without perturbing other elements of the dpp expression pattern (Glise and Noselli, 1997;Hou et al, 1997;Riesgo-Escovar and Hafen, 1997).…”

Section: Introductionmentioning

confidence: 99%

Stress signaling in Drosophila

1999

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“…Dpp is a secreted signaling molecule of the transforming growth factor ␤ (TGF-␤) family (Padgett et al 1987). Two Dpp receptors, Thick vein (Tkv) and Punt (Put), have been identified in flies, as well as a number of components acting downstream of these receptors, including Mad, Medea, and the Zinc finger protein Schnurri (Brummel et al 1994;Nellen et al 1994;Penton et al 1994;Grieder et al 1995;Letsou et al 1995;Ruberte et al 1995;Stronach and Perrimon 1999). Loss-of-function mutations in hep, bsk, DJun, and DFos all lead to severe DC defects that are characterized by a complete failure of the entire lateral ectoderm, including the LE cells, to elongate dorsally.…”

Section: Dorsal Closure In Drosophila As a Model System For Wound Repairmentioning

confidence: 99%