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Hi Tim,I think it does the grouping of features based on the Target value and so it thinks there's a long intron there rather than it being intergenic space.best,~b
On Tue, Oct 10, 2017 at 4:44 PM, falinor181 <falin...@gmail.com> wrote:
Hi there,I'm troubleshooting a gene prediction issue in evidence modeler where two nearby homologous genes are getting fused into one extra long gene with a long intronic spacer in between. Weights are as follows:PROTEIN protein2genome 4TRANSCRIPT blat-Ppyr1.3_Pasa_v1 5TRANSCRIPT gmap-Ppyr1.3_Pasa_v1 5OTHER_PREDICTION maker 1ABINITIO_PREDICTION transdecoder 20The "transdecoder" features are derived from the PASA pipeline. Overall, my logic for these weights are to strongly rely on the transcript derived gene models, while only relying on the ab-initio a little to help capture some more genes / decrease fragmented genes.I've found for this particular locus, the transdecoder GFF seems to have captured the two loci properly. I think the issue may be the protein/transcript evidence I am providing. Does EVM chain together the transcript/protein evidence based on the "Target" attribute of the GFF features? I'm noticing that some of my protein evidence via exonerate spans both genes. Although,I have filtered out those "protein_match" features that span both genes, I've noticed that the "match_part" features on either gene do have the same "Target" attribute...All the best,-Tim
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