CLOCKWORK ORANGE Enhances PERIOD Mediated Rhythms in Transcriptional Repression by Antagonizing E-box Binding by CLOCK-CYCLE

Earlier studies demonstrated that cwo mRNA cycles in phase with per, tim, vri, and Pdp1, but with a higher basal level, and thus lower amplitude [9,12–14]. To determine whether CWO protein levels also cycle, western analysis was carried out using head extracts from wild-type flies collected every 4 hours in a 12-h light/12-h dark (LD) cycle. We find that the levels of CWO do not change throughout an LD cycle (Fig 1), consistent with previous results [15]. Given that cwo mRNA levels cycle, it is possible that constant CWO levels result from post-transcriptional regulation or a long half-life.

CWO contains a bHLH domain, a structural motif that characterizes a family of E-box binding transcription factors [16–19], which suggests that CWO may regulate CLK-CYC target gene transcription via E-box binding. Previous ChIP-on-chip and gel-shift analyses in S2 cells demonstrated that CWO specifically binds to the E-box of core clock genes [12,13], however it is still unknown whether CWO binds those core clock genes in vivo, and whether the binding intensity changes throughout the day. To test these possibilities, ChIP assays were carried out on wild-type flies collected in the early morning (ZT2) and in the early night (ZT14) using CWO and CLK antisera. Fragments containing upstream E-boxes from tim, per, Pdp1 and vri, which are necessary for high-amplitude mRNA cycling in vitro or in vivo [4,5,20–25], were amplified from the immunoprecipitates and then quantified. In CWO immunoprecipitates, the tim, vri and Pdp1 E-box containing fragments were two to threefold more abundant at ZT2 than at ZT14 (Fig 2A), suggesting that CWO binding is time-dependent, though the dynamic binding of CWO on the per E-box fragment is less robust than the others. Importantly, this temporal binding pattern is antiphase to CLK binding, as CLK shows high binding intensity during the night at ZT14 and low binding during the daytime at ZT2 (Fig 2B), consistent with previous results [8,11].

The reciprocal binding pattern of CLK and CWO implies that these transcription factors compete for E-box binding. If so, both CLK and CWO must occupy the same E-boxes. To test this possibility, we determined how mutating E-boxes upstream of tim affected CLK and CWO binding. The circadian enhancer upstream of tim is comprised of two tandem E-boxes that are spaced seven nucleotides apart [24,26], a structure that is conserved among core clock genes in various species [27]. Both of these E-boxes were indispensable for tim mRNA expression in S2 cells [24], suggesting that these tandem E-box motifs are binding sites for both CLK and CWO. To determine if this is the case, a series of 136bp fragments from the tim promoter containing an E-box1 (E1) mutant (mE1-E2), an E-box 2 (E2) mutant (E1-mE2), an E1 and E2 double mutant (mE1-mE2) or a control with wild-type E-boxes (E1-E2) were generated, inserted into the pHPdestGFP vector [28], and targeted to the attP18 genomic site (Fig 3A).

To confirm that this promoter fragment is sufficient to drive rhythmic expression, we carried out quantitative reverse transcription-PCR (qRT-PCR) to monitor GFP mRNA levels in flies collected every 4-h during an LD cycle. Quantification of GFP mRNA levels in flies with WT tim promoter shows a ~10-fold diurnal rhythm with a peak at ZT14 and a trough at ZT2 to ZT6 (S1 Fig), consistent with timing and amplitude of per and tim mRNA cycling in wild-type flies [29,30]. However, even at the normal tim mRNA peak (ZT14), mE1-E2, E1-mE2 and mE1-mE2 flies express little or no eGFP mRNA (S1 Fig), indicating that both E1 and E2 are indispensable for expression of tim mRNA in vivo. This result is consistent with previous tim-luciferase reporter results in S2 cells [24].

We next carried out ChIP assays using CWO and CLK antisera on the same fly strains to test whether E1 and E2 are required for CWO and CLK binding. At ZT2, when CWO strongly binds to the tim promoter, CWO binding intensity was drastically reduced in mE1-E2, E1-mE2 and mE1-mE2 flies compared to WT (Fig 3B). Likewise, CLK binding intensity was drastically reduced in mE1-E2, E1-mE2 and mE1-mE2 flies compared to WT at ZT14, when CLK binding is strongest (Fig 3B). These results indicate that both E1 and E2 are indispensable for both CWO and CLK binding to the tim circadian enhancer. Given that CWO specifically targets E-boxes in S2 cells by Gel-shift analyses [13], we conclude that both CLK and CWO bind intact tandem E1-E2 motifs in vivo. In mice, CLK-BMAL1 dimers cooperatively bind tandem E-boxes in vitro [27,31], and this may be the case for CWO given the requirement for both E1 and E2 E-boxes.

Previous studies showed that increasing the level of CWO expression reduces per, tim, vri and Pdp1ɛ mRNA levels in S2 cells and that their trough mRNA levels are higher in cwo mutant or knockdown flies, indicating that CWO acts to repress CLK-mediated gene transcription in vitro and in vivo [9,12–14]. Given that CWO and CLK bind to the same E-box motif, we wondered whether CWO represses CLK-mediated transcription by inhibiting CLK binding. To test this possibility, ChIP assays were carried out using CLK antiserum on wild-type and cwo⁵⁷⁰³ flies at the trough (ZT2) and peak (ZT14) times of CLK-CYC target gene transcription and mRNA abundance in LD. Although cwo⁵⁷⁰³ mutants lengthen the period of activity rhythms by 2–3h in DD [9,13], the peak and trough phases of CLK-CYC target gene transcription and mRNA abundance are comparable in cwo⁵⁷⁰³ mutants and wild-type flies in LD [9,13]. We find that CLK binds tim E-boxes with a robust rhythm in wild-type flies and a lower amplitude rhythm in the cwo⁵⁷⁰³ mutant (Fig 4A). However, the intensity of CLK binding in cwo⁵⁷⁰³ is significantly increased at ZT2 compared to wild-type, indicating that CWO acts to reduce CLK-CYC binding at the trough of its binding cycle (Fig 4B). Given that CWO strongly binds tim E-boxes at ZT2 (Fig 2A), we propose that CWO inhibits CLK-CYC binding during the repression phase by antagonizing PER-CLK-CYC complexes to maintain off-DNA repression. There was no significant difference in CLK binding between cwo⁵⁷⁰³ and wild-type at ZT14 (Fig 4B), despite decreased peak levels of per, tim, vri and Pdp1ɛ mRNA at ZT14 in cwo mutant and RNAi knockdown flies [9,12–14], suggesting that CWO has little impact on CLK-CYC binding in the absence of PER.

Given that CWO suppresses CLK binding at ZT2 in the early morning but not at ZT14 during the early evening (Fig 4B), it is possible that PER is necessary for CWO to antagonize CLK E-box binding since PER accumulates to high levels in the nucleus around dawn and is at low levels in the cytoplasm around dusk [32]. Indeed, our results support a model developed previously to explain cooperation between CWO and PER to repress CLK-CYC mediated transcription in S2 cells [9]. In this model, CWO is proposed to compete with CLK-CYC heterodimers for E-box binding only when PER binds CLK-CYC, thereby reducing their affinity for E-box binding. To test this model, we performed ChIP assays using CWO antiserum on wild-type, Clk^out and per¹ flies collected at ZT2 and ZT14 in LD. In Clk^out flies, which necessarily lack CLK-CYC heterodimers [33], CWO is bound to tim E-boxes at both ZT2 and ZT14 with binding signals comparable to the strong CWO binding in wild-type flies at ZT14 (Fig 5A). In contrast, in per¹ flies, which lack PER-dependent repression of CLK-CYC activation [34], low binding signals of CWO were detected at ZT2 and ZT14, indicating that PER is indeed required for CWO to bind E-boxes (Fig 5A). Moreover, CWO binding was significantly increased in Clk^out versus wild-type flies at ZT14, indicating that CLK-CYC binding at ZT14 reduces CWO binding. Likewise, a significant increase in CWO binding was also seen in wild-type versus per¹ flies at ZT2, indicating that PER enhances CWO binding (Fig 5A).

To determine whether differences in CWO binding in Clk^out and per¹ flies were due to differences in CWO protein levels, we carried out western analysis using head extracts from these mutants collected at ZT2 and ZT14. Since cwo transcription is regulated in part by the transcriptional feedback loop, CWO protein levels are slightly lower in Clk^out flies and slightly higher in per¹ flies (Fig 5B and 5C). However, the lower levels of CWO in Clk^out resulted in higher E-box binding, and higher CWO protein levels in per¹ resulted in lower E-box binding. This result suggests that the differences in CWO-E-box binding are not due to altered CWO protein levels, but due to the relative DNA binding affinities of CWO and CLK in these mutants. These results, taken together, strongly support and extend the model described by Kadener et al., 2007, for CWO binding as it relates to CLK-CYC repression. When CLK-CYC targets are activated, CLK-CYC binds DNA with higher affinity than CWO, thus CLK binding is not altered in the presence or absence of CWO. When CLK-CYC targets are repressed, PER binds CLK-CYC complexes and decreases their DNA binding affinity, thereby favoring CWO binding to E-boxes and enhancing PER mediated removal of CLK-CYC-PER complexes from the DNA (Fig 6). Although we can’t exclude the possibility that PER enables CWO E-box binding independent of its interaction with CLK-CYC, the available evidence strongly supports the model proposed.

DNA fragments containing wild-type or mutant E-boxes from the upstream tim circadian enhancer were used to construct GFP-reporter transgenes. These 136bp fragments extend from -578 to -714 relative to the tim transcription start site, and contain “E1-E2” E-box motifs that are wild-type (E1-E2), E1 mutant (mE1-E2), E2 mutant (E1-mE2) or E1-E2 mutant (mE1-mE2). These wild-type and mutant E-box fragments were generated by PCR amplification using the following primer sets: E1-E2, 5’-CACCTTTGGCAAATAAACGTGCGGCA-3’ and 5’-TGCCGGCGTTTGTGCGAA-3’; mE1-E2, 5’-CACCTTTGGCAAATAAACGTGCGGCACGTTGTGATTAAGATCTAGCCGAT-3’ and 5’-TGCCGGCGTTTGTGCGAA-3’; E1-mE2, 5’-CACCTTTGGCAAATAAGATCTCGGAGATTTGTGATTACACGTGAGCCGAT-3’ and 5’-TGCCGGCGTTTGTGCGAA-3’; mE1-mE2, 5’-CACCTTTGGCAAATAAGATCTCGGAGATTTGTGATTAAGATCTAGCCGAT-3’ and 5’-TGCCGGCGTTTGTGCGAA-3’. The PCR products were inserted into the pENTR/D-TOPO vector using pENTR Directional TOPO cloning kit (Invitrogen), and then subcloned into the pHPdesteGFP vector, which expresses Green Fluorescent Protein (GFP) according to the enhancer sequence inserted [28], using Gateway LR-Clonase System (Invitrogen). The nucleotide sequences of all transgenes were confirmed by sequencing. The resulting transgenes were injected into embryos (BestGene) for recombination into the attp18 genomic site via PhiC31-mediated transgenesis to yield tim circadian enhancer GFP (tim-CEG) flies [52–54].

Flies were entrained in a 12-h light/12-h dark (LD) incubator for at least 3 days, collected at the indicated time points, and frozen. Isolated frozen fly heads were homogenized in radioimmunoprecipitation assay (RIPA) buffer (20 mM Tris at pH 7.5, 150 mM NaCl, 1 mM EDTA, 0.05 mM EGTA, 10% glycerol, 1% Triton X-100, 0.4% sodium deoxycholate) containing 0.5 mM PMSF (phenylmethylsulfonyl fluoride), 10 μg/ml aprotinin, 10 μg/ml leupeptin, 2 μg/ml pepstatin A, 1 mM Na₃VO₄, and 1 mM NaF. This homogenate was sonicated 3 to 5 times for 10 s each time, using a Misonix XL2000 model sonicator at a setting of 3 and then centrifuged at 20,000 g for 10 min. The supernatant was collected as RIPA S extract, and protein concentration was determined by the Bradford assay. Equal amounts of RIPA S extract were run, transferred, and probed with guinea pig anti-CWO (GP-27), 1:5,000 and mouse anti-beta-actin (Abcom), 1:20,000. Horseradish peroxidase-conjugated secondary antibodies (Sigma) against guinea pig and mouse were diluted 1:5,000. Immunoblots were visualized using ECL plus (GE) reagent. Protein levels were measured by placing a rectangle of the same size over each CWO, ß-Actin or non-specific (NS) protein band on films used to visualize the immunoblots, and quantifying the signal within each rectangle via densitometric analysis using the ImageJ program. The levels of CWO were calculated as a CWO:ß-Actin or CWO:NS ratio, and CWO abundance at each time point was plotted relative to wild-type at ZT2.

Chromatin IP (ChIP) assays and qPCR quantification were performed as previously described [55]. CLK and CWO binding to E-boxes in the circadian enhancers upstream of tim, per, vri, and Pdp1 in wild-type flies and the circadian enhancer in tim-CEG flies were first quantified via qPCR, and the resulting values were corrected for nonspecific binding to an intergenic region on chromosome 3R (nucleotides 29576172 to 29576303). The primers used for qPCR were as follows: for tim E-boxes, 5’-ACACTGACCGAAACACCCACTC-3’ and 5’-GCGGCACGTTGTGATTACACG-3’; for per E-boxes, 5’-GGGTGAGTAATGCCGTTGCGAAAT-3’ and 5’-ATTTGCTGGCCAAGTCACGCAGTT-3’; for vri E-boxes, 5’-CTGGTGCCTCACATTCCACG-3’ and 5’- CAGCAGTCAAGTTATAGCAGCGC-3’; for Pdp1 E-boxes, 5’-GCACTCTCATTCTCTCTGTCGC-3’ and 5’-ACTTGGGGGACTGGAACTG-3’; for tim-CEG, 5’-GCCCCCTTCACCTTTGGCAAATA-3’ and 5’-TACAAGAAAGCTGGGTCGGCG-3’; and for the intergenic region, 5’-CAGGAGTCGVAGGACCAACC-3’ and 5’-GTCCTGAGAGGCTGAGAGGC-3’. PCR amplification using each pair of primers produced a single band of the expected size. The tim-CEG primers target vector sequences that flank the genomic tim E-box insert, and thus do not amplify endogenous tim genomic sequences.

Quantitative RT-PCR was performed as described [55,56], with some modifications, to measure GFP mRNA levels. Total RNA was isolated from frozen fly heads using Trizol (Invitrogen), and treated with a Turbo DNase DNA-free kit (Ambion) to eliminate genomic DNA contamination. DNA-free total RNA (1.0 μg) was reverse transcribed using oligo(dT) 12–28 primers (Invitrogen) and Superscript II (Invitrogen). The reverse transcription (RT) product was amplified with SsoFast qPCR Supermix (Bio-Rad) in a Bio-Rad CFX96 Real-Time PCR System using primers to GFP (5’-TACGGCAAGCTGACCCTGAAGT-3’ and 5’-CGCACCATCTTCTTCAAGGACG-3’) and ribosomal protein 49 (rp49) (5’-TACAGGCCCAAGATCGTGAA-3’ and 5’-GCACTCTGTTGTCGATACCC-3’). For each sample, mRNA quantity was determined using the standard curve for each gene analyzed. To determine the relative levels of GFP mRNA over a diurnal cycle, GFP mRNA levels were divided by rp49 mRNA levels for each time point and plotted as the GFP/rp49 mRNA ratio. To quantify GFP mRNA in different tim-CEG strains at the wild-type (E1-E2) peak, GFP/rp49 values were normalized to the E1-E2 value at ZT14.

All relevant data are within the paper and its Supporting Information files.