Expression of an S phase-stabilized version of the CDK inhibitor Dacapo can alter endoreplication

Swanson, Christina I.; Meserve, Joy H.; McCarter, Patrick C.; Alexis, Thieme,; Tony, Mathew,; Elston, Timothy C.; Duronio, Robert J.

doi:10.1242/dev.115006

Cited by 19 publications

(20 citation statements)

References 67 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Dap is a member of the mammalian p21 family of cyclin-dependent kinase inhibitors (CKIs) and inhibits the G1-to-S phase transition by sequestering the CycE/Cdk2 complex in a stable but inactive form (Lane et al, 1996). Induction of dap transcription causes a rapid accumulation of Dap protein, which inhibits CycE/Cdk2 activity and leads to G1 cell cycle arrest (Swanson et al, 2015). Conversely, dap knockdown leads to tissue hypertrophy and cancer processes (Kiyokawa et al, 1996; Nakayama et al, 1996).…”

Section: Resultsmentioning

confidence: 99%

Myoglianin triggers the pre-metamorphosis stage in hemimetabolan insects

Kamsoi

Bellés

2018

Preprint

View full text Add to dashboard Cite

show abstract

Section: Resultsmentioning

confidence: 99%

Myoglianin triggers the pre-metamorphosis stage in hemimetabolan insects

Kamsoi

Bellés

2018

Preprint

View full text Add to dashboard Cite

show abstract

“…Dap is a member of the mammalian p21 family of cyclin-dependent kinase inhibitors and inhibits the G1-to-S phase transition by sequestering the CycE/Cdk2 complex in a stable but inactive form (31). Induction of dap transcription causes a rapid accumulation of Dap protein, which inhibits CycE/Cdk2 activity and leads to G1 cell cycle arrest (32). Conversely, dap knockdown leads to tissue hypertrophy and cancer processes (33,34).…”

Section: Myo Depletion Causes Cell Hyperproliferation In the Pgmentioning

confidence: 99%

Myoglianin triggers the premetamorphosis stage in hemimetabolan insects

Kamsoi

Bellés

2018

FASEB j.

View full text Add to dashboard Cite

Insect metamorphosis is triggered by a decrease in juvenile hormone (JH) in the final juvenile instar. What induces this decrease is therefore a relevant question. Working with the cockroach Blattella germanica, we found that myoglianin (Myo), a ligand in the TGF‐β signaling pathway, is highly expressed in the corpora allata (CA, the JH‐producing glands) and the prothoracic gland [(PG), which produce ecdysone] during the penultimate (fifth) nymphal instar (N5). In the CA, high Myo levels during N5 repress the expression of juvenile hormone acid methyl transferase, a JH biosynthesis gene. In the PG, decreasing JH levels trigger gland degeneration, regulated by the factors Krüppel homolog 1, FTZ‐F1, E93, and inhibitor of apoptosis‐1. Also in the PG, a peak of myo expression in N5 indirectly stimulates the expression of ecdysone biosynthesis genes, such as neverland, enhancing the production of the metamorphic ecdysone pulse in N6. The Myo expression peak in N5 also represses cell proliferation, which can enhance ecdysone production. The data indicate that Myo triggers the premetamorphic nymphal instar in B. germanica and possibly in other hemimetabolan insects.—Kamsoi, O., Belles, X. Myoglianin triggers the premetamorphosis stage in hemimetabolan insects. FASEB J. 33, 3659–3669 (2019). http://www.fasebj.org

show abstract

“…In CycE high and G1-FUCCI negative S phase cells, Dap expression is almost undetectable and therefore no longer coupled to CycE (Figure 3D arrowhead). This is likely due to the PIP box-dependent degradation of Dap, by CRL4 Cdt2 in S phase [26]. This result suggests that Dap is expressed in CycE high G phase cells to limit its activity prior to entering S phase.…”

Section: Dap Sets the Cyce/cdk2 Activity Threshold For Timely S Phasementioning

confidence: 94%

E2F-dependent genetic oscillators control endoreplication

Kim

Moon

2019

Preprint

View full text Add to dashboard Cite

Polyploidy is an integral part of development and is associated with cellular stress, aging and pathological conditions. The endoreplication cycle, comprised of successive alternations of G and S phases without cell division, is widely employed to produce polyploid cells. The endocycle is driven by continuous oscillations of Cyclin E/Cdk2 activity, which is governed by E2F transcription factors. In this study, we provide mechanistic insight on how E2F-dependent Cdk oscillations during endocycles are maintained in Drosophila salivary glands. Genetic experiments revealed that an alternative splicing isoform of E2F1, E2F1b, regulates the circuitry of timely S phase entry and exit by activating a subset of E2F target genes. E2F1b regulates the Drosophila ortholog of p27 CIP/KIP -like Cdk inhibitor Dacapo to precisely time S phase entry by controlling the CycE/Cdk2 activity threshold. Upon entry to S phase, E2F1bdependent PCNA expression establishes a negative feedback loop through the PIP box-mediated degradation of E2F1. Overall, our study uncovers a network of E2Fdependent genetic oscillators that are critical for the periodic transition between G and S phases during endoreplication.

show abstract

Expression of an S phase-stabilized version of the CDK inhibitor Dacapo can alter endoreplication

Cited by 19 publications

References 67 publications

Myoglianin triggers the pre-metamorphosis stage in hemimetabolan insects

Myoglianin triggers the pre-metamorphosis stage in hemimetabolan insects

Myoglianin triggers the premetamorphosis stage in hemimetabolan insects

E2F-dependent genetic oscillators control endoreplication

Contact Info

Product

Resources

About