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  <docDscr>
    <citation>
      <titlStmt>
        <titl xml:lang="sv">RNA-sekvensering av kombinationsbehandling med SL-176 och GSK-J4 i neuroblastomcellinjer</titl>
        <parTitl xml:lang="en">RNA sequencing of drug combinations for SL-176 and GSK-J4 in neuroblastoma cell lines</parTitl>
        <IDNo agency="SND">2025-72-1</IDNo>
        <IDNo agency="ki.se">Not applicable</IDNo>
        <IDNo agency="DOI">https://doi.org/10.48723/rkz9-n137</IDNo>
      </titlStmt>
      <prodStmt>
        <producer xml:lang="en" abbr="SND">Swedish National Data Service</producer>
        <producer xml:lang="sv" abbr="SND">Svensk nationell datatjänst</producer>
      </prodStmt>
      <holdings URI="https://doi.org/10.48723/rkz9-n137">Landing page</holdings>
    </citation>
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  <stdyDscr>
    <citation>
      <titlStmt>
        <titl xml:lang="sv">RNA-sekvensering av kombinationsbehandling med SL-176 och GSK-J4 i neuroblastomcellinjer</titl>
        <parTitl xml:lang="en">RNA sequencing of drug combinations for SL-176 and GSK-J4 in neuroblastoma cell lines</parTitl>
        <IDNo agency="SND">2025-72-1</IDNo>
        <IDNo agency="ki.se">Not applicable</IDNo>
        <IDNo agency="DOI">https://doi.org/10.48723/rkz9-n137</IDNo>
        <IDNo agency="SwePub">oai:swepub.ki.se:1023018</IDNo>
        <IDNo agency="DOI">10.1038/s41419-025-07658-1</IDNo>
      </titlStmt>
      <rspStmt>
        <AuthEnty xml:lang="en" affiliation="Department of Women's and Children's Health, Karolinska Institutet">Treis, Diana</AuthEnty>
        <AuthEnty xml:lang="sv" affiliation="Institutionen för kvinnors och barns hälsa, Karolinska Institutet">Treis, Diana</AuthEnty>
        <AuthEnty xml:lang="en" affiliation="Department of Women's and Children's Health, Karolinska Institutet">Wickström Näsman, Malin</AuthEnty>
        <AuthEnty xml:lang="sv" affiliation="Institutionen för kvinnors och barns hälsa, Karolinska Institutet">Wickström Näsman, Malin</AuthEnty>
      </rspStmt>
      <prodStmt />
      <distStmt>
        <distrbtr xml:lang="en" abbr="SND" URI="https://snd.se">Swedish National Data Service</distrbtr>
        <distrbtr xml:lang="sv" abbr="SND" URI="https://snd.se">Svensk nationell datatjänst</distrbtr>
        <distDate xml:lang="en" date="2025-03-31" />
      </distStmt>
      <verStmt>
        <version elementVersion="1" elementVersionDate="2025-03-31" />
      </verStmt>
      <holdings URI="https://doi.org/10.48723/rkz9-n137">Landing page</holdings>
    </citation>
    <stdyInfo>
      <subject>
        <keyword xml:lang="en" vocab="ELSST" vocabURI="https://elsst.cessda.eu/id/6/13d01f0e-44ed-4f28-9ef6-7046a6fe0322">CANCER</keyword>
        <keyword xml:lang="sv" vocab="ELSST" vocabURI="https://elsst.cessda.eu/id/6/13d01f0e-44ed-4f28-9ef6-7046a6fe0322">CANCER</keyword>
        <keyword xml:lang="en" vocab="ELSST" vocabURI="https://elsst.cessda.eu/id/6/533b3769-3715-484f-a781-9b0a3422f51f">PHARMACOLOGY</keyword>
        <keyword xml:lang="sv" vocab="ELSST" vocabURI="https://elsst.cessda.eu/id/6/533b3769-3715-484f-a781-9b0a3422f51f">FARMAKOLOGI</keyword>
        <keyword xml:lang="en" vocab="MeSH" vocabURI="http://id.nlm.nih.gov/mesh/D009447">Neuroblastoma</keyword>
        <keyword xml:lang="sv" vocab="MeSH" vocabURI="http://id.nlm.nih.gov/mesh/D009447">Neuroblastom</keyword>
        <keyword xml:lang="en" vocab="MeSH" vocabURI="http://id.nlm.nih.gov/mesh/D010372">Pediatrics</keyword>
        <keyword xml:lang="sv" vocab="MeSH" vocabURI="http://id.nlm.nih.gov/mesh/D010372">Pediatrik</keyword>
        <keyword xml:lang="en" vocab="MeSH" vocabURI="http://id.nlm.nih.gov/mesh/D010600">Pharmacology</keyword>
        <keyword xml:lang="sv" vocab="MeSH" vocabURI="http://id.nlm.nih.gov/mesh/D010600">Farmakologi</keyword>
      </subject>
      <abstract xml:lang="en" contentType="abstract">High-risk neuroblastoma remains a deadly disease with a survival rate of only 50-60 %. Prognosis is particularly poor in children who relapse after chemotherapy. In light of this, increasing attention has been directed toward the development of targeted therapies for neuroblastoma.

Drug combination screening and follow-up experiments have shown that the WIP1 inhibitor SL-176 and the H3K27 demethylase inhibitor GSK-J4 act synergistically against neuroblastoma cells. To understand the mechanisms behind this synergism, we have treated cells of neuroblastoma cell lines IMR-32 and SK-N-BE(2) with either vehicle, SL-176, GSK-J4, or the combination of both drugs for 72 hours and performed RNA sequencing (Illumina NextSeq 550).

Total RNA was subjected to quality control with the Agilent TapeStation (Agilent Technologies, Santa Clara, CA, USA) according to the manufacturer’s instructions. To construct libraries suitable for Illumina sequencing, the Illumina TruSeq Stranded mRNA sample preparation protocol which includes mRNA isolation, cDNA synthesis, ligation of adapters and amplification of indexed libraries was used. The yield and quality of the amplified libraries was analyzed using Qubit by ThermoFisher and the Agilent TapeStation. The indexed cDNA libraries were normalized and combined, and the pools were sequenced on the Illumina NextSeq 550 (Illumina, San Diego, CA, USA) for a 75-cycle v2 sequencing run generating 75 bp single-end reads. Basecalling and demultiplexing was performed using CASAVA software (Illumina) with default settings generating Fastq files for further downstream mapping and analysis. Raw data was adapter and quality trimmed using Cutadapt, and aligned to the human genome build (Gene reference: Ensembl Homo_sapiens.GRCh38.104.gtf) using STAR. Gene assignment was performed using FeatureCounts. Differential gene expression was determined using DEseq2.</abstract>
      <abstract xml:lang="sv" contentType="abstract">Läkemedelskombinationsscreening och uppföljande experiment har visat att WIP1-hämmaren SL-176 och H3K27-demethylashämmaren GSK-J4 verkar synergistiskt i neuroblastomceller. För att förstå mekanismerna bakom denna synergism har vi behandlat celler från neuroblastom-cellinjerna IMR-32 och SK-N-BE(2) med antingen vehikel, SL-176, GSK-J4 eller en kombination av båda läkemedlen i 72 timmar och genomfört RNA-sekvensering (Illumina NextSeq 550).

För ytterligare beskrivning av RNA-sekvensering och dataanalys, se beskrivning på engelska.</abstract>
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        <anlyUnit xml:lang="en" unit="Cells">Cells<concept vocab="DDI Analysis Unit" vocabURI="https://vocabularies.cessda.eu/v2/vocabularies/AnalysisUnit/2.1.3?languageVersion=en-2.1.3">Cells</concept></anlyUnit>
        <anlyUnit xml:lang="sv" unit="Celler">Celler<concept vocab="DDI Analysis Unit" vocabURI="https://vocabularies.cessda.eu/v2/vocabularies/AnalysisUnit/2.1.3?languageVersion=sv-2.1.3">Celler</concept></anlyUnit>
        <universe xml:lang="en">Human cell lines SK-N-BE(2) (#CRL-2271, ATCC) and IMR-32 (#CCL-127, ATCC) exposed for experimental compounds.</universe>
        <universe xml:lang="sv">Humana cellinjer SK-N-BE(2) (#CRL-2271, ATCC) och IMR-32 (#CCL-127, ATCC) exponerade för experimentella substanser.</universe>
        <dataKind xml:lang="en">Numeric</dataKind>
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    <method>
      <dataColl>
        <sampProc xml:lang="en">The cell lines are commercially available and were purchased from ATCC (American Type Culture Collection), www.atcc.org. The data includes no personal information.<concept vocab="DDI Sampling Procedure" vocabURI="https://vocabularies.cessda.eu/v2/vocabularies/SamplingProcedure/2.0.1?languageVersion=en-2.0.1">The cell lines are commercially available and were purchased from ATCC (American Type Culture Collection), www.atcc.org. The data includes no personal information.</concept></sampProc>
        <sampProc xml:lang="sv">Cellinjerna finns kommersiellt tillgängliga och är köpta från ATCC (American Type Culture Collection), www.atcc.org. Data innehåller inte några personuppgifter.<concept vocab="DDI Sampling Procedure" vocabURI="https://vocabularies.cessda.eu/v2/vocabularies/SamplingProcedure/2.0.1?languageVersion=sv-2.0.1">Cellinjerna finns kommersiellt tillgängliga och är köpta från ATCC (American Type Culture Collection), www.atcc.org. Data innehåller inte några personuppgifter.</concept></sampProc>
        <sampProc xml:lang="en">Other<concept vocab="DDI Sampling Procedure" vocabURI="https://vocabularies.cessda.eu/v2/vocabularies/SamplingProcedure/2.0.1?languageVersion=en-2.0.1">Other</concept></sampProc>
        <sampProc xml:lang="sv">Övrigt<concept vocab="DDI Sampling Procedure" vocabURI="https://vocabularies.cessda.eu/v2/vocabularies/SamplingProcedure/2.0.1?languageVersion=sv-2.0.1">Övrigt</concept></sampProc>
      </dataColl>
    </method>
    <dataAccs>
      <useStmt>
        <restrctn xml:lang="en">Access to data through SND. Data are freely accessible.</restrctn>
        <restrctn xml:lang="sv">Åtkomst till data via SND. Data är fritt tillgängliga.</restrctn>
        <conditions elementVersion="info:eu-repo-Access-Terms vocabulary">openAccess</conditions>
      </useStmt>
    </dataAccs>
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      <relPubl>
        <citation>
          <titlStmt>
            <titl xml:lang="sv">Treis, D., Lundberg, K.I., Bell, N. et al. Targeted inhibition of WIP1 and histone H3K27 demethylase activity synergistically suppresses neuroblastoma growth. Cell Death Dis 16, 318 (2025). https://doi.org/10.1038/s41419-025-07658-1</titl>
            <parTitl xml:lang="en">Treis, D., Lundberg, K.I., Bell, N. et al. Targeted inhibition of WIP1 and histone H3K27 demethylase activity synergistically suppresses neuroblastoma growth. Cell Death Dis 16, 318 (2025). https://doi.org/10.1038/s41419-025-07658-1</parTitl>
            <IDNo agency="DOI">10.1038/s41419-025-07658-1</IDNo>
            <IDNo agency="SWEPUB">oai:swepub.ki.se:1023018</IDNo>
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            <distDate date="2025">2025</distDate>
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