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US20240006029A1 - Systems and methods for predicting therapy efficacy from normalized biomarker scores - Google Patents

Systems and methods for predicting therapy efficacy from normalized biomarker scores
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US20240006029A1
US20240006029A1US18/460,330US202318460330AUS2024006029A1US 20240006029 A1US20240006029 A1US 20240006029A1US 202318460330 AUS202318460330 AUS 202318460330AUS 2024006029 A1US2024006029 A1US 2024006029A1
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therapy
biomarker
expression
level
scores
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Alexander Bagaev
Feliks Frenkel
Ravshan Ataullakhanov
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BostonGene Corp
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BostonGene Corp
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Assigned to BOSTONGENE, LLCreassignmentBOSTONGENE, LLCASSIGNMENT OF ASSIGNORS INTEREST (SEE DOCUMENT FOR DETAILS).Assignors: BAGAEV, Alexander, FRENKEL, Feliks, ATAULLAKHANOV, RAVSHAN
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Abstract

Techniques for determining therapy scores for at least two of an anti-PD1 therapy, an anti-CTLA4 therapy, an IL-2 therapy, an IFN alpha therapy, an anti-cancer vaccine therapy, an anti-angiogenic therapy, and an anti-CD20 therapy. The techniques include determining, using sequencing data for the subject and information indicating distribution of biomarker values across one or more reference populations, a first set of normalized biomarker scores for a first set of biomarkers associated with a first therapy; and a second set of normalized biomarker scores for a second set of biomarkers associated with a second therapy; providing the first set of normalized biomarker scores as input to a statistical model to obtain a first therapy score for the first therapy; and providing the second set of normalized biomarker scores as input to the statistical model to obtain a second therapy score for the second therapy.

Description

Claims (21)

31. A method, comprising:
using at least one computer hardware processor to perform:
obtaining sequencing data previously obtained by sequencing at least one biological sample of a subject;
obtaining biomarker information for multiple biomarkers including a first biomarker, each biomarker of the multiple biomarkers being associated with at least one therapy of multiple therapies, the first biomarker being associated with a first therapy of the multiple therapies, wherein the biomarker information includes, for each particular biomarker of the multiple biomarkers, a respective distribution of values for the particular biomarker, the biomarker information including a first distribution of values for the first biomarker;
determining, using the sequencing data, multiple biomarker scores including a respective biomarker score for each of at least some of the multiple biomarkers, the multiple biomarker scores including a first biomarker score for the first biomarker;
normalizing the multiple biomarker scores to a common scale using at least some of the biomarker information, thereby obtaining multiple normalized biomarker scores for the subject, the normalizing comprising:
normalizing the first biomarker score using the first distribution of values for the first biomarker to obtain a first normalized biomarker score for the subject;
determining therapy scores for at least some therapies of the multiple therapies using the multiple normalized biomarker scores, the determining comprising:
determining a first therapy score for the first therapy using at least some of the multiple normalized biomarker scores including the first normalized biomarker score; and
recommending, for the subject, at least one therapy of the at least some therapies based on the determined therapy scores,
wherein the at least one therapy is selected from the group consisting of: an anti-PD1 therapy, an anti-CTLA4 therapy, an IL-2 therapy, an IFN alpha therapy, an anti-cancer vaccine therapy, an anti-angiogenic therapy, and an anti-CD20 therapy.
wherein Table 2 is:TherapyBiomarkersaPD1Affinity ofAXLB2M LOFBRAFtherapyneontigensmutationmutationBRCA2 mutationCancer gene panelsCancer gene panelsCCL13(CGPs) FM-CGP(CGPs) HSL-CGPCCL2CCL7CCL8CD8+ cell density inthe tumor invasivemarginCD8+ cell numberCDH1CVEGFCCX3CL1 expressionCXCR2 expressionDendritic cell numberEGFR expressionEndothelial cellsEosinophil numberESRP1 expressionFibroblastsGranzyme BexpressionJAK1 LOF mutationJAK2 LOF mutationLDH levelLymphocyte numberM1 macrophageM1/M2 macrophageMDSC %MHC-II expressionnumberratioMHC-II expressionMissmatch-repairMITF expressionMutational Burden(HLA-DRA)deficiency statusPattern of distantPD-L1 expressionPD-L1 expression onPTEN lossmetastasesinfiltrating leukocytesQuantity ofROR2STAT1 expressionT reg cell %neoantigen peptidesTAGLNTCR clonalityTGFbeta levelTIL number intumorTWIST2VEGF levelVEGFAaCTLA4AbsoluteCD8+ cell numberCXCL11 expressionCXCL9 expressiontherapylymphocyte countCXCR3 expressionDendritic cell numberEOMES + CD8+ cellsFOXP3+ cellsnumbernumberIDO expressionLDH expressionM1 macrophageM1/M2 macrophagenumberratioMDSC %Mutational BurdenNY-ESO-1 seropostivePTEN lossT reg cell %TCR clonalityTGFbeta levelTIL number intumorVEGF levelIL-2 therapyBone metastasisconcomitant regionalLeucocytes numberLNPEP expressionlymphadenopathyC-reactive proteinDelta32 CCR5BCAT2 expressionBDNFOSlevelPolymorphismexpressionIL-10 (−1082G -> A)CAIX expressionLOC130576CCR5 LOFpolymorphismexpressionmutationERCC1 (codon 118)IFN-g (+874A -> T)LOC399900ATP6V0A2polymorphismpolymorphismexpressionexpressionKi-67 expressionAlkaline phosphataseARHGAP10CD56+ or CD57+levelexpressioncells numberLiver metastasisCD83+ TIDC cellsCDNA FLJ37989LDH levelnumberexpressionFibronectin levelHLA-DQB1GBF1 expressionamount of alveolarexpressioncomponentAlbumin levelclear cellFOXP3+ cells numberHLA-DQA1histologyexpressiongranular featuresMAP3K5 expressionMDSC numberMediastinummetastasisMEF2A expressionMTUS1 expressionNeutrophil numberNK cell numbernon clear cellNR1H2 expressionNRAS mutationsNumber ofhistologymetastatic sitespapillary featuresPH-4 expressionPlatelets NumberRABL2BexpressionRC3H2 expressionrs12553173Sedimentation rateSUPT6HexpressionTACC1 expressionTDP1 expressionTFPI expressionTime from tumor tooccurrence ofmetastasesTransferrin levelTSH levelVCAM1 expressionVEGF levelWeight lossα-antitrypsin levelIFNaCAIX levelDelta32 CCR5Leucocytes countLNPEP expressiontherapyPolymorphismERCC1 (codon 118)GBF1 expressionBone metastasisBreslow thicknesspolymorphismIL-6 expressionCCR5 LOF mutationLOC130576CD4+ cells numberlevelexpressionHepatic RIG-1IL-1ß expressionLOC399900BDNFOSexpressionlevelexpressionexpressionInterval from initialARHGAP10BCAT2 expressionCD8+ CD57+ cellsdiagnosis toexpressionnumbertreatmentLiver metastasisCD83+ TIDC cellscDNA FLJ37989 fisKi-67 expressionnumberexpressionHLA-Cw06 alleleIL-1α expressionHLA-DQB1ATP6V0A2levelexpressionexpressionAlkalinecollagen IV levelHLA-DQA1IL-10 (-1082G -> A)phosphatase levelexpressionpolymorphismIFN-g (+874A -> T)MAP3K5 expressionMediastinum metastasisMEF2A expressionpolymorphismMIP-1α expressionMIP-1ß expressionMTAP gene expressionMTUS1 expressionlevellevelNeutrophil countNR1H2 expressionNumber of metastaticOsteopontin levelsitesPerformance statusPH-4 expressionPlatelets NumberRABL2BexpressionRC3H2 expressionSedimentation rateSerum calcium levelSerum hemoglobinlevelSTAT1 geneSUPT6H expressionTACC1 expressionTDP1 expressionexpressionTFP1 expressionTime from tumor toTNF-α expression levelTRAIL leveloccurrence ofmetastasesUlceration ofVCAM1 expressionVEGF levelVEGFR2 levelprimaryAnti-cancerCancer-TestisCD16 + CD56 + CD69 +CD4 + CD45RO + cellCD4 + CTLA-4 + TvaccineAntigens' Geneslymphocytesnumbercell numbertherapyexpressionnumberCD4 + PD-1 + T cellC-reactive proteinECOG performanceEGF levelnumberlevelscoreI/II high-grade or IIIIFN-gamma-inducedIgM for Blood Group AIL-6 levelT1/2/3a low-gradetumor cell apoptosistrisaccharide leveldisease intermediateriskIntratumoral versusLDH levelLin-CD14 + HLA-DR-/lymphocyte numberperitumoral T celllo MDSC leveldensitylymphocytes inM1/M2 macrophageMDSC numberMean CorpuscularPBMC %ratioHemoglobinConcentration(MCHC)Number of CD27-Patient's agePredictive genePTEN lossCD45RA+ andsignature in MAGE A3CD27-CD45RA-antigen-specific cancerandimmunotherapyCD27+CD45RA- T-cellsSerum amyloid ASerum S100BSyndecan-4 mRNAT reg cell %levelconcentrationexpression levelTGFbeta levelToll-like receptor 4WT1 expressiongene polymorphismAnti-Acneiform rashAdrenomedullinangiopoietin-2Bioactive PeptideangiogenicRepeatexpression levelsInduced SignalingtherapyPolymorphismPathwayCD133 expressionCDC16 levelChild-Pugh classCXCL10 plasmalevelCXCR1 rs2234671CXCR2 C785TCXCR2 rs2230054ECOG PerformanceG > CT > CStatusEGF A-61GEGF rs444903 A > GEGFR expression levelsEGFR rs2227983G > AEndothelin-1Expression of CD31Expression of PDGFR-HBV statusexpression levelsbetaHGF plasma levelHistory of alcoholICAM1 T469CIFN-α2 plasma levelintakeIGF-1 rs6220 A > GIL-12 plasma levelIL-16 plasma levelIL-2Rα plasma levelIL-3 plasma levelIL-6 plasma levelIL-8 251 T > AIL-8 plasma levelLck and FynLiver metastasisM-CSF plasma levelmucinous histologytyrosine kinases ininitiation of TCRActivation pathwayactivationNO2-dependent ILNumber of restingNumber of totalPIGF plasma level12 Pathwaycirculatingcirculating endothelialactivation in NKendothelial cellscellscellsportal veinrs12505758 inrs2286455rs3130thrombosisVEGFR2rs699946 in VEGFASDF-1 α plasma levelSexsVEGFR1T Cell ReceptorT Helper Cell SurfaceTRAIL plasma levelVEGF -1154 A > GSignaling PathwayMolecules expressionactivationVEGF-1498 C > TVEGF C936TVEGF G-634CVEGF-1154 G/AVEGF-2578 C/AVEGFR1 rs9582036VEGFR-2 rs2305948WNK1-rs11064560C > TRituximabBCL2 expressionBCL6 expressionBeclin-1 expressionC1qA GenelevelPolymorphismCarbohydrateCD163-positiveCD20 expressionCD37 expressionantigen-125 levelmacrophageslevelCD5 expressionCXCR4 expressionCytotoxic TFcγRIIIa 158H/Hlevellevellymphocyte-associatedgenotypesGranzyme B expressionlevelGalectin-1HIP1R mRNA levelIL-12 levelIL-1RA levelexpressionKi-67 expressionMARCO expressionMast cell number 1miR-155 expressionMYC expressionNumber ofp21 protein expressionsLR11 levelmacrophagesSMAD1 expressionSTAT3T cellsTAM numbermRNA levelTIM3 expression
obtaining sequencing data about at least one biological sample of a subject;
obtaining sequencing data previously obtained by sequencing at least one biological sample of a subject;
obtaining biomarker information for multiple biomarkers including a first biomarker, each biomarker of the multiple biomarkers being associated with at least one therapy of multiple therapies, the first biomarker being associated with a first therapy of the multiple therapies, wherein the biomarker information includes, for each particular biomarker of the multiple biomarkers, a respective distribution of values for the particular biomarker, the biomarker information including a first distribution of values for the first biomarker;
determining, using the sequencing data, multiple biomarker scores including a respective biomarker score for each of at least some of the multiple biomarkers, the multiple biomarker scores including a first biomarker score for the first biomarker;
normalizing the multiple biomarker scores to a common scale using at least some of the biomarker information, thereby obtaining multiple normalized biomarker scores for the subject, the normalizing comprising:
normalizing the first biomarker score using the first distribution of values for the first biomarker to obtain a first normalized biomarker score for the subject;
determining therapy scores for at least some therapies of the multiple therapies using the multiple normalized biomarker scores, the determining comprising:
determining a first therapy score for the first therapy using at least some of the multiple normalized biomarker scores including the first normalized biomarker score; and
recommending, for the subject, at least one therapy of the at least some therapies based on the determined therapy scores,
wherein the at least one therapy is selected from the group consisting of: an anti-PD1 therapy, an anti-CTLA4 therapy, an IL-2 therapy, an IFN alpha therapy, an anti-cancer vaccine therapy, an anti-angiogenic therapy, and an anti-CD20 therapy.
46. At least one non-transitory computer-readable storage medium storing processor-executable instructions that, when executed by at least one computer hardware processor, causes the at least one computer hardware processor to perform a method, comprising:
obtaining sequencing data previously obtained by sequencing at least one biological sample of a subject;
obtaining biomarker information for multiple biomarkers including a first biomarker, each biomarker of the multiple biomarkers being associated with at least one therapy of multiple therapies, the first biomarker being associated with a first therapy of the multiple therapies, wherein the biomarker information includes, for each particular biomarker of the multiple biomarkers, a respective distribution of values for the particular biomarker, the biomarker information including a first distribution of values for the first biomarker;
determining, using the sequencing data, multiple biomarker scores including a respective biomarker score for each of at least some of the multiple biomarkers, the multiple biomarker scores including a first biomarker score for the first biomarker;
normalizing the multiple biomarker scores to a common scale using at least some of the biomarker information, thereby obtaining multiple normalized biomarker scores for the subject, the normalizing comprising:
normalizing the first biomarker score using the first distribution of values for the first biomarker to obtain a first normalized biomarker score for the subject;
determining therapy scores for at least some therapies of the multiple therapies using the multiple normalized biomarker scores, the determining comprising:
determining a first therapy score for the first therapy using at least some of the multiple normalized biomarker scores including the first normalized biomarker score; and
recommending, for the subject, at least one therapy of the at least some therapies based on the determined therapy scores,
wherein the at least one therapy is selected from the group consisting of: an anti-PD1 therapy, an anti-CTLA4 therapy, an IL-2 therapy, an IFN alpha therapy, an anti-cancer vaccine therapy, an anti-angiogenic therapy, and an anti-CD20 therapy.
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