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PIONEERING CANCER RESEARCH
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Breast
BCM-0132
Model Details
Patient
PDX Model
Histology
Metastasis
Patient Treatment
Patient Information for Model: BCM-0132
Contact Model Developer
Model Contact
Model: BCM-0132
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-0132
Model Details - Initial Implantation of Patient Tissue
Biomarkers & Mutations
Model Details - Acceptable Conditions for Passaging
Mutations (Cancer Gene Census List)
Show/Hide Columns
The number of models in this collection with mutations in the listed gene;
may include models that are not publicly available for distribution.
The number of models in this collection with mutations at the listed site;
may include models that are not publicly available for distribution.
Total mutations showing: 276
F
P
1
2
3
4
5
6
7
8
9
10
N
E
Rows Per Page
10
15
25
50
Download
Gene
Filter by Gene
Chr
Filter by Chr
Start
End
Ref
Alt
cDNA Change
Codon Change
Protein Change
TVAF
Gene Mutation Freq.
Site Mutation Freq.
Most Severe Effect
All Effects
Mutation Impact
Transcript ID
ClinVar Clinical Significance
COSMIC ID
gnomAD Non-Cancer AF
dbSNP ID
Gene Mutation Freq.
Site Mutation Freq.
Transcript ID
ClinVar Clinical Significance
COSMIC ID
dbSNP ID
ABL1
chr9
130884102
130884105
CAAG
C
c.1826_1828del
AAG/-
p.K609del
0.018
55
42
In-frame Deletion
In-frame Deletion
MODERATE
ENST00000318560.6
COSV59324524
rs201725154
55
42
ENST00000318560.6
COSV59324524
rs201725154
AFF4
chr5
132897083
132897103
GTGTAGCTATTCCCAGTGCCC
G
c.1527_1546del
caGGGCACTGGGAATAGCTACAct/cact
p.Q509Hfs*2
0.535
20
1
Frameshift Mutation
Frameshift Mutation
HIGH
ENST00000265343.10
.
20
1
ENST00000265343.10
.
AKAP9
chr7
92085597
92085597
C
T
c.8935C>T
Cct/Tct
p.P2979S
0.971
115
115
Missense Variant
Missense Variant
MODERATE
ENST00000356239.8
Benign/Likely_benign
COSV104663065
0.996325000000
rs1063242
115
115
ENST00000356239.8
Benign/Likely_benign
COSV104663065
rs1063242
ALK
chr2
29193706
29193706
T
C
c.4381A>G
Atc/Gtc
p.I1461V
0.037
115
115
Missense Variant
Missense Variant
MODERATE
ENST00000389048.8
Benign
COSV101201052
0.997594000000
rs1670283
115
115
ENST00000389048.8
Benign
COSV101201052
rs1670283
APC
chr5
112841059
112841059
T
A
c.5465T>A
gTc/gAc
p.V1822D
0.969
100
100
Missense Variant
Missense Variant
MODERATE
ENST00000257430.9
Benign
COSV57321643
0.794920000000
rs459552
100
100
ENST00000257430.9
Benign
COSV57321643
rs459552
AR
chrX
67545316
67545316
T
TGCAGCAGCAGCA
c.228_239dup
ctg/ctGCAGCAGCAGCAg
p.Q77_Q80dup
0.923
101
8
In-frame Insertion
In-frame Insertion
MODERATE
ENST00000374690.9
.
101
8
ENST00000374690.9
.
AR
chrX
67546514
67546517
TGGC
T
c.1418_1420del
GGC/-
p.G473del
0.894
101
11
In-frame Deletion
In-frame Deletion
MODERATE
ENST00000374690.9
COSV65958513
.
101
11
ENST00000374690.9
COSV65958513
.
ARID1A
chr1
26696761
26696761
C
T
c.358C>T
Ccg/Tcg
p.P120S
0.94
48
2
Missense Variant
Missense Variant
MODERATE
ENST00000324856.13
Conflicting_interpretations_of_pathogenicity
COSV61373973
0.000271628000
rs571264557
48
2
ENST00000324856.13
Conflicting_interpretations_of_pathogenicity
COSV61373973
rs571264557
ARID1B
chr6
157206530
157206534
CTGTT
C
c.5763_5766del
cTGTTt/ct
p.F1921Lfs*52
0.976
80
1
Frameshift Mutation
Frameshift Mutation
HIGH
ENST00000636930.2
COSV99269679
rs1554237269
80
1
ENST00000636930.2
COSV99269679
rs1554237269
ATR
chr3
142562770
142562770
A
G
c.632T>C
aTg/aCg
p.M211T
0.972
101
91
Missense Variant
Missense Variant
MODERATE
ENST00000350721.9
Benign/Likely_benign
COSV63383325
0.545488000000
rs2227928
101
91
ENST00000350721.9
Benign/Likely_benign
COSV63383325
rs2227928
BCL6
chr3
187728423
187728423
C
T
c.1477G>A
Gct/Act
p.A493T
0.606
39
34
Missense Variant
Missense Variant
MODERATE
ENST00000406870.7
not_provided
COSV51650064
0.141440000000
rs2229362
39
34
ENST00000406870.7
not_provided
COSV51650064
rs2229362
BCLAF1
chr6
136278255
136278255
G
C
c.626C>G
tCc/tGc
p.S209C
0.5
114
114
Missense Variant
Missense Variant
MODERATE
ENST00000531224.6
COSV62140211
rs6940018
114
114
ENST00000531224.6
COSV62140211
rs6940018
BCR
chr22
23285182
23285182
A
G
c.2387A>G
aAt/aGt
p.N796S
0.947
104
99
Missense Variant
Missense Variant
MODERATE
ENST00000305877.13
Benign
COSV59932309
0.812555000000
rs140504
104
99
ENST00000305877.13
Benign
COSV59932309
rs140504
BCR
chr22
23309463
23309463
A
G
c.3052A>G
Acc/Gcc
p.T1018A
0.069
104
19
Missense Variant
Missense Variant
MODERATE
ENST00000305877.13
COSV59933861
0.000222703000
rs746213513
104
19
ENST00000305877.13
COSV59933861
rs746213513
BIRC6
chr2
32488639
32488639
A
T
c.8020A>T
Act/Tct
p.T2674S
0.903
100
93
Missense Variant
Missense Variant
MODERATE
ENST00000421745.6
Benign
COSV70195673
0.588029000000
rs2366894
100
93
ENST00000421745.6
Benign
COSV70195673
rs2366894
Total mutations showing: 276
F
P
1
2
3
4
5
6
7
8
9
10
N
E
Rows Per Page
10
15
25
50
Download
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-0132
Patient
PDX
ER
HER2
PR
Metastasis Information for Model: BCM-0132
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-0132
Event Id
Treatment
Treatment Setting
Age at Start
Age at End
Duration
Clinical Response
Pathologic Response
Reason Stopped
20
Cyclophosphamide,Doxorubicin
Neoadjuvant
58.92
59.0
29 days
Partial Response
Not Reported
Treatment Completed
25
Carboplatin,Paclitaxel
Neoadjuvant
59.09
59.34
91 days
Complete Response
Partial Response
Treatment Completed
35
Docetaxel
Adjuvant
59.46
59.63
62 days
Not Reported
Not Applicable
Treatment Completed
40
Radiation Therapy
Adjuvant
59.76
59.84
29 days
Not Reported
Not Applicable
Treatment Completed
45
Capecitabine
Adjuvant
59.95
60.4
164 days
Stable Disease
Not Applicable
Treatment Completed
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