TY - JOUR
T1 - A juvenile hormone agonist reveals distinct developmental pathways mediated by ecdysone-inducible Broad Complex transcription factors
AU - Restifo, Linda L.
AU - Wilson, Thomas G.
PY - 1998
Y1 - 1998
N2 - Juvenile hormone (JH) is an important regulator of insect development that, by unknown mechanisms, modifies molecular, cellular, and organismal responses to the molting hormone, 20-hydroxyecdysone (20E). In dipteran insects such as Drosophila, JH or JH agonists, administered at times near the onset of metamorphosis, cause lethality. We tested the hypothesis that the JH agonist methoprene acts by interfering with function of the Broad Complex (BRC), a 20E-regulated locus encoding BTB/POZ-zinc finger transcription factors essential for metamorphosis of many tissues. We found that methoprene, administered by feeding or by topical application, disrupts the metamorphic reorganization of the central nervous system, salivary glands, and musculature in a dose-dependent manner. As we predicted, methoprene phenocopies a subset of previously described BRC defects; it also phenocopies Deformed and produces abnormalities not associated with known mutations. Interestingly, methoprene specifically disrupts those metamorphic events dependent on the combined action of all BRC isoforms, while sparing those that require specific isoform subsets. Thus, our data provide independent pharmacological evidence for the model, originally based on genetic studies, that BRC proteins function in two developmental pathways. Mutations of Methoprene-tolerant (Met), a gene involved in the action of JH, protect against all features of the 'methoprene syndrome.' These findings have allowed us to propose novel alternative models linking BRC, juvenile hormone, and MET.
AB - Juvenile hormone (JH) is an important regulator of insect development that, by unknown mechanisms, modifies molecular, cellular, and organismal responses to the molting hormone, 20-hydroxyecdysone (20E). In dipteran insects such as Drosophila, JH or JH agonists, administered at times near the onset of metamorphosis, cause lethality. We tested the hypothesis that the JH agonist methoprene acts by interfering with function of the Broad Complex (BRC), a 20E-regulated locus encoding BTB/POZ-zinc finger transcription factors essential for metamorphosis of many tissues. We found that methoprene, administered by feeding or by topical application, disrupts the metamorphic reorganization of the central nervous system, salivary glands, and musculature in a dose-dependent manner. As we predicted, methoprene phenocopies a subset of previously described BRC defects; it also phenocopies Deformed and produces abnormalities not associated with known mutations. Interestingly, methoprene specifically disrupts those metamorphic events dependent on the combined action of all BRC isoforms, while sparing those that require specific isoform subsets. Thus, our data provide independent pharmacological evidence for the model, originally based on genetic studies, that BRC proteins function in two developmental pathways. Mutations of Methoprene-tolerant (Met), a gene involved in the action of JH, protect against all features of the 'methoprene syndrome.' These findings have allowed us to propose novel alternative models linking BRC, juvenile hormone, and MET.
KW - Broad Complex
KW - Central nervous system
KW - Deformed
KW - Drosophila
KW - Ecdysone
KW - Juvenile hormone
KW - Met
KW - Metamorphosis
KW - Methoprene
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U2 - 10.1002/(SICI)1520-6408(1998)22:2<141::AID-DVG4>3.0.CO;2-6
DO - 10.1002/(SICI)1520-6408(1998)22:2<141::AID-DVG4>3.0.CO;2-6
M3 - Article
C2 - 9581286
AN - SCOPUS:0031920343
SN - 0192-253X
VL - 22
SP - 141
EP - 159
JO - Developmental Genetics
JF - Developmental Genetics
IS - 2
ER -