PDX INSIGHTS
PIONEERING CANCER RESEARCH
Model Details

Patient Information for Model: BCM-0046

Model Contact
Model: BCM-0046
Model Contact: Michael Lewis
Institution: BCM Breast PDX Program
Email: mtlewis@bcm.edu

Patient Information
Clinical Timeline

Color Keys:
 
 Positive
 
 Negative
 
 N/A

Clinical Information at Collection
Clinical Biomarkers/Mutations at Collection
Pathology Information at Collection

Model Information for Model: BCM-0046

Model Details - Initial Implantation of Patient Tissue
Biomarkers & Mutations
Model Details - Acceptable Conditions for Passaging
Mutations (Cancer Gene Census List)

GeneChrStartEndRefAltcDNA ChangeCodon ChangeProtein ChangeTVAF Gene Mutation Freq. Site Mutation Freq.Most Severe EffectAll EffectsMutation ImpactTranscript IDClinVar Clinical SignificanceCOSMIC IDgnomAD Non-Cancer AFdbSNP IDGene Mutation Freq.Site Mutation Freq.Transcript IDClinVar Clinical SignificanceCOSMIC IDdbSNP ID
AKAP9chr79208559792085597CTc.8935C>TCct/Tctp.P2979S0.967115115Missense VariantMissense VariantMODERATEENST00000356239.8
Benign/Likely_benign
COSV104663065
0.996325000000rs1063242
115115ENST00000356239.8Benign/Likely_benignCOSV104663065rs1063242
ALDH2chr12111789845111789845ATc.463A>TAag/Tagp.K155*0.81341Nonsense MutationNonsense MutationHIGHENST00000261733.7


.
41ENST00000261733.7.
ALKchr22919350029193500GCc.4587C>GgaC/gaGp.D1529E0.99211580Missense VariantMissense VariantMODERATEENST00000389048.8
Benign
COSV66569695
0.472160000000rs1881421
11580ENST00000389048.8BenignCOSV66569695rs1881421
ALKchr22919370629193706TCc.4381A>GAtc/Gtcp.I1461V0.993115115Missense VariantMissense VariantMODERATEENST00000389048.8
Benign
COSV101201052
0.997594000000rs1670283
115115ENST00000389048.8BenignCOSV101201052rs1670283
ALKchr22919361529193615TCc.4472A>GaAg/aGgp.K1491R0.99211551Missense VariantMissense VariantMODERATEENST00000389048.8
Benign
COSV66555753
0.349007000000rs1881420
11551ENST00000389048.8BenignCOSV66555753rs1881420
ASXL1chr203243640432436404CTc.3692C>TtCc/tTcp.S1231F0.317405Missense VariantMissense VariantMODERATEENST00000375687.10
Benign
COSV105900478
0.021269300000rs74638057
405ENST00000375687.10BenignCOSV105900478rs74638057
ATRXchrX7768247177682471CGc.2785G>CGag/Cagp.E929Q0.9239173Missense VariantMissense VariantMODERATEENST00000373344.10
Benign

rs3088074
9173ENST00000373344.10Benignrs3088074
AXIN2chr176555847365558473GAc.148C>TCct/Tctp.P50S0.9947560Missense VariantMissense VariantMODERATEENST00000307078.10
Benign
COSV61057354
0.474888000000rs2240308
7560ENST00000307078.10BenignCOSV61057354rs2240308
BAP1chr35240450052404500ACc.1203T>GtaT/taGp.Y401*0.94281Nonsense MutationNonsense MutationHIGHENST00000460680.6
Conflicting_interpretations_of_pathogenicity

0.000149294000rs200156887
81ENST00000460680.6Conflicting_interpretations_of_pathogenicityrs200156887
BAP1chr35240450252404502ACc.1201T>GTat/Gatp.Y401D0.94381Missense VariantMissense VariantMODERATEENST00000460680.6
Uncertain_significance

0.000149312000rs376563004
81ENST00000460680.6Uncertain_significancers376563004
BARD1chr2214809500214809500GAc.70C>TCcc/Tccp.P24S0.9698552Missense VariantMissense VariantMODERATEENST00000260947.9
Benign
COSV53608734
0.384797000000rs1048108
8552ENST00000260947.9BenignCOSV53608734rs1048108
BAZ1Achr143479278234792782GTc.1503C>AgaC/gaAp.D501E0.382151Missense VariantMissense VariantMODERATEENST00000360310.6


.
151ENST00000360310.6.
BCLAF1chr6136278255136278255GCc.626C>GtCc/tGcp.S209C0.234114114Missense VariantMissense VariantMODERATEENST00000531224.6

COSV62140211
rs6940018
114114ENST00000531224.6COSV62140211rs6940018
BCRchr222328518223285182AGc.2387A>GaAt/aGtp.N796S0.90110499Missense VariantMissense VariantMODERATEENST00000305877.13
Benign
COSV59932309
0.812555000000rs140504
10499ENST00000305877.13BenignCOSV59932309rs140504
BIRC6chr23248863932488639ATc.8020A>TAct/Tctp.T2674S0.94110093Missense VariantMissense VariantMODERATEENST00000421745.6
Benign
COSV70195673
0.588029000000rs2366894
10093ENST00000421745.6BenignCOSV70195673rs2366894
CNV

PDX Validation
In order to validate the identity of Baylor College of Medicine patient-derived xenograft (PDX) models, short tandem repeat (STR) testing is performed at the Cytogenetics and Cell Authentication core facility at MDACC. STR testing is performed on tissue from the initial tumor grown in the mouse (transplant generation 1 - TG1) and from a patient sample when possible. Thereafter, STR testing is performed every five transplant generations (TG5, TG10, TG15, and TG20). In the case that a PDX model is transplanted from viably frozen tissue to restart the model, the PDX Core will test the first outgrowth to confirm identity and every five transplant generations thereafter. In addition to STR, we assess clinical biomarkers and histology every 5th transplant generation. Finally, RNAseq gene expression profiles are evaluated periodically to ensure consistency with previous results and to evaluate phenotypic drift. If a significant change in PDX biology is noted, we identify the last known stable stock and re-start the model.

Histology Information for Model: BCM-0046
Patient
PDX

Metastasis Information for Model: BCM-0046
 
Patient
PDX
Abdomen
Adrenal gland
Bone
Bones
Brain
CTC
Chest
Chest wall
Contralateral Breast
Dura
Fallopian Tubes
Head
Kidney
Liver
Lung
Lymph node
Lymph nodes
Neck
Ovary
Pancreas
Pericardium
Peritoneal cavity
Peritoneum
Pleura
Pleural effusion
Shoulder
Skin
Spine
Spleen
Thoracic Spine
Thymus

Patient Treatment Information for Model: BCM-0046

Event IdTreatmentTreatment SettingAge at StartAge at EndDurationClinical ResponsePathologic ResponseReason Stopped
15Cyclophosphamide,EpirubicinNeoadjuvant53.5853.7666 daysPartial ResponseNot ApplicableTreatment Completed
20DocetaxelNeoadjuvant53.8153.9966 daysStable DiseasePartial ResponseTreatment Completed
30Radiation Therapy Adjuvant54.254.3347 daysNot ReportedNot ApplicableTreatment Completed













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