Validation cohort
We collected 29 new cases and 19 new controls as validation cohort.
Case dataset
Median age at diagnosis was 57 years (range 39 - 76); the majority of cases were categorized as serous carcinomas (25/29, 86%) and all cases were high grade (G3) (29/29, 100%). According to FIGO classification, 2 cases (7%) were stage II, 19 (65.5%) stage III and 8 (27.5%) stage IV.
Twenty-two out of 29 cases (76%) were treated with up-front surgery; seven (24%) received neo-adjuvant chemotherapy (NACT) followed by Interval Debulking Surgery (IDS). Residual tumor was present in 18 cases (62%), absent in 11 (38%).
All cases relapsed, with a median PFS of 15 months (range 0-62). Median age at diagnosis of CNS involvement was 59 years, with a median bPFS of 25 months (range 0-87 months). Fourteen out of 29 (48%) patients developed brain metastases as the first site of relapse.
Overall, median bOS was 17 months (range 2-112), while median OS was 48 months (range 4-173). At the time statistical analyses were performed (May 2018), 7/29 patients (24%) were alive, while 22 (76%) had died.
Table 1 shows the most relevant clinico-pathological parameters of cases subgroup of the validation cohort.
Table 1 Clinico-pathological features of primary ovarian lesion in validation cohort: case dataset vs control dataset
|
Clinico-histopathological features validation cohort
|
Case Dataset
n=29 (%)
|
Control Dataset
n=19 (%)
|
p Value
|
Age, median (years) [range]
|
57[39-76]
|
52[40-78]
|
N.S.
|
Histological type
Serous
Clear cell
Undifferentiated
Other
|
25 (86)
2 (7)
1 (3)
1 (3)
|
19 (100)
|
N.S.
|
Histological grade
G3
|
29 (100)
|
19 (100)
|
N.S.
|
FIGO stage
II
III
IV
|
2 (7)
19 (65.5)
8 (27.5)
|
0 (0)
13 (68)
6 (32)
|
N.S.
|
Type of surgery
Upfront
Neoadjuvant CT + IDS
|
22 (76)
7 (24)
|
8 (42)
11 (58)
|
0.02
|
Macroscopic residual tumor
Present
Absent
|
18 (62)
11 (38)
|
6 (32)
13 (68)
|
0.04
|
First-line chemotherapy
|
|
|
|
Platinum-based
|
29 (100)
|
19 (100)
|
N.S.
|
Relapse
Present
Absent
|
29 (100)
|
12 (63)
7 (37)
|
0.0004
|
First site of relapse
CNS
Lymph nodes and / or peritoneum
Other
|
14 (48)
11 (38)
4 (14)
|
0 (0)
11 (92)*
1 (8)*
|
0.003
|
Patient’s status
Alive
Dead
|
7 (24)
22 (76)
|
15 (79)
4 (21)
|
0.0002
|
PFS, median (months) [range]
|
15 [0-62]
|
17 [10-62]
|
N.S.
|
OS, median (months) [range]
|
48 [4-173]
|
32 [19-78]
|
N.S.
|
|
*Disease progression did not occur for 7 patients.
IDS: Interval Debulking Surgery; CT: Chemotherapy; CNS: Central Nervous System; PFS: Progression Free Survival; OS: Overall Survival; N.S.: not significant.
|
For more detailed features of CNS involvement in the combined dataset see Table 2.
Table 2 Clinical parameters of the 40 CNS metastases included in the study
|
Cases
|
Age
|
Neurological symptoms
|
N° of lesions
|
Site of lesions
|
Treatment of CNS metastases
|
bPFS (months)
|
bOS (months)
|
PREVIOUSLY PUBLISHED COHORT
|
1
|
49
|
NA
|
Single
|
Parietal
|
Surgery, CT
|
11
|
6
|
2
|
57
|
Drowsiness
|
Single
|
Occipital
|
Surgery
|
68
|
42
|
3
|
70
|
Ataxia
|
Single
|
Parietal, occipital
|
Surgery, WBRT
|
29
|
41
|
4
|
70
|
Unilateral symptoms
|
Single
|
Parietal
|
Surgery, CT, WBRT
|
22
|
6
|
5
|
50
|
Headache, vertigo
|
Double
|
Parietal, occipital, frontal
|
Surgery, CT, WBRT
|
18
|
29
|
6
|
70
|
Aphasia, disorientation, dizziness
|
Single
|
Parietal
|
Surgery, SRS
|
28
|
56
|
7
|
52
|
NA
|
Single
|
Frontal
|
Surgery, CT, WBRT
|
54
|
7
|
8
|
62
|
Headache, altered walking gait
|
Multiple
|
Temporal, frontal, occipital
|
Surgery, WBRT
|
15
|
3
|
9
|
46
|
NA
|
Single
|
NA
|
Surgery
|
23
|
3
|
10
|
72
|
Ataxia, dysmetria
|
Multiple
|
Frontal (major)
|
Surgery, WBRT
|
18
|
7
|
11
|
74
|
Vertigo
|
Single
|
Frontal
|
Surgery, WBRT
|
25
|
64
|
VALIDATION COHORT
|
12
|
56
|
Seizures, aphasia, altered walking gait
|
Single
|
Frontal
|
Surgery, WBRT
|
0
|
48
|
13
|
77
|
Persistent vomiting
|
Single
|
Cerebellar
|
Surgery
|
26
|
40
|
14
|
79
|
Dysarthria, altered walking gait
|
Single
|
Parietal
|
Surgery
|
36
|
6
|
15
|
66
|
Paresthesia, dizziness
|
Multiple
|
Parietal, occipital
|
Surgery, CT, SRS
|
30
|
34
|
16
|
69
|
Seizures, dysmetria
|
Single
|
Frontal
|
Surgery
|
0
|
12
|
17
|
67
|
Headache, diplopia
|
Single
|
Occipital
|
Surgery, CT
|
45
|
12
|
18
|
67
|
Headache, vomit
|
Single
|
Frontal
|
Surgery, WBRT
|
22
|
40
|
19
|
68
|
Headache
|
Single
|
Frontal
|
Surgery, WBRT
|
26
|
27
|
20
|
56
|
Aphasia, seizures, dysarthria, dysmetria
|
Multiple
|
Temporal, parietal, occipital
|
Surgery, CT, WBRT
|
61
|
112
|
21
|
57
|
Headache, vomit
|
Single
|
Cerebellar
|
Surgery, WBRT
|
18
|
41
|
22
|
60
|
Altered walking gait
|
Multiple
|
Cerebellar, supratentorial
|
Surgery, CT, WBRT
|
19
|
13
|
23
|
54
|
Headache, paresthesia, hemiparesis
|
Multiple
|
Temporal, parietal
|
Surgery, CT, WBRT
|
15
|
44
|
24
|
46
|
Altered walking gait
|
Single
|
Cerebellar
|
Surgery, WBRT
|
25
|
8
|
25
|
69
|
Altered walking gait, dizziness, Hemianopia
|
Multiple
|
Parietal, occipital
|
Surgery, WBRT
|
22
|
39
|
26
|
71
|
Headache
|
Double
|
Frontal, Cerebellar
|
WBRT, CT
|
32
|
27
|
27
|
51
|
Aphasia, verbal amnesia
|
Multiple
|
Frontal, temporal, occipital
|
WBRT
|
34
|
6
|
28
|
59
|
Headache, altered walking gait
|
Multiple
|
Cerebellar, supratentorial
|
WBRT
|
25
|
18
|
29
|
74
|
Altered walking gait, diplopia
|
Multiple
|
Cerebellar, parietal, temporal
|
WBRT
|
87
|
17
|
30
|
58
|
Seizures
|
Multiple
|
Cerebellar, supratentorial
|
WBRT
|
16
|
22
|
31
|
78
|
NA
|
Multiple
|
supratentorial
|
WBRT
|
27
|
2
|
32
|
60
|
NA
|
Double
|
Temporal, frontal
|
WBRT, CT
|
36
|
44
|
33
|
75
|
Asthenia, fatigue
|
Multiple
|
Cerebellar, supratentorial
|
WBRT, CT
|
21
|
3
|
34
|
51
|
Headache
|
Multiple
|
Parietal, occipital
|
WBRT, CT
|
72
|
8
|
35
|
54
|
NA
|
Single
|
Occipital
|
WBRT
|
1
|
3
|
36
|
49
|
Hemiparesis
|
Multiple
|
Frontal, temporal, occipital
|
SRS
|
28
|
51
|
37
|
39
|
Paresthesia, Dysarthria
|
Multiple
|
Occipital, cerebellar
|
WBRT, CT
|
4
|
4
|
38
|
55
|
Drowsiness
|
Multiple
|
Parietal, frontal
|
/
|
38
|
2
|
39
|
57
|
Headache, Paresthesia
|
Multiple
|
Frontal, parietal, occipital
|
WBRT, CT
|
1
|
15
|
40
|
55
|
Headache
|
Multiple
|
Frontal, cerebellar
|
WBRT, CT
|
11
|
9
|
|
|
|
|
|
|
|
|
|
|
NA: not available; WBRT: Whole Brain RadioTherapy; SRS: Stereotactic RadioSurgery; CT: Chemotherapy; bPFS: Progression Brain Metastasis Free Survival; bOS: brain metastases Overall Survival
|
Control dataset
The median age of primary EOC diagnosis was 52 years (range 40-78). All our controls were high grade (G3) serous carcinomas (19/19, 100%). There were 13 FIGO stage III (68%) and 6 FIGO stage IV (32%). Eleven out of 19 patients (58%) were treated with neoadjuvant chemotherapy followed by IDS. Up-front surgery was chosen for 8 women (42%), followed by adjuvant chemotherapy. All patients received platinum-based chemotherapy (19/19, 100). Thirteen patients (68%) had no residual tumor after surgery. Twelve controls (63%) experienced at least one relapse of the disease. Median PFS was 17 months (range 10-62), whereas median OS was 32 months (range 19-78). When data were processed, 4 (21%) patients had died.
Table 1 shows the most relevant clinico-pathological parameters of control subgroup.
Cases and controls of the validation cohort were comparable: no statistical difference was observed for age, histotype, tumor grade, FIGO stage, and first line chemotherapy (see Table 1). Significant differences between two group were observed for upfront surgery vs interval cytoreductive surgery, absence/presence of residual tumor after surgery, incidence of relapse and number of surviving patients.
AR expression in cases and controls of the validation cohort
Immune-histochemical stainings were performed on both cases and controls of the validation cohort. Table 3 (see below) shows comparisons between cases vs controls, considered as continuous variables.
Table 3 Immune-histochemical results and statistical analyses of AR considered as continuous variable: comparisons of cases vs controls in validation cohort
|
IHC parameter
|
Cases vs controls
(%)
|
N
|
Mean
(%)
|
Median (%)
|
Range
|
p Value
|
|
|
|
|
|
|
|
AR
|
Cases
|
29
|
13.21
|
5
|
0 - 70
|
< 0.001
|
Controls
|
19
|
43.21
|
40
|
1 - 95
|
|
|
|
|
|
|
|
|
|
|
AR: Androgen Receptor
|
For AR protein expression in cases and controls of the validation cohort as dichotomized variable see Table 4 (see below).
Table 4 Immune-histochemical results and statistical analyses of AR considered as dichotomized variable as for both cases and controls validation datasets
|
IHC parameter
|
Cut-off
|
Case dataset (primary ovarian lesions)
(%)
|
Control dataset (primary ovarian lesions)
(%)
|
p Value
(Cases vs controls: IHC comparison)
|
OR
(Cases vs controls)
(CI 95%)
|
|
|
|
|
|
|
AR
|
< 1%
|
4/29 (13.8)
|
0/19 (0)
|
0.142
|
|
≥ 1%
|
25/29 (86.2)
|
19/19 (100)
|
|
< 10%
|
20/29 (69)
|
4/19 (21.1)
|
0.003
|
8,33 (2.15 - 32.29)
|
≥ 10%
|
9/29 (31)
|
15/19 (78.9)
|
IRS ≤ 2
|
24/29 (82.8)
|
4/19 (21.1)
|
< 0.001
|
|
IRS > 2
|
5/29 (17.2)
|
15/19 (78.9)
|
|
|
|
|
|
|
|
|
AR: Androgen Receptor
|
AR expression is significantly reduced in cases vs controls’ validation cohort
Case dataset vs. control dataset. AR shows a statistically significant difference between the subgroups when considered as continuous variable (mean case dataset: 13.21%; mean control dataset: 43.21%, p<0.001, see Table 3).
Moreover, considered as dichotomized variable, different expression of AR among the two populations emerges (p=0.003 for10% cut-off and p<0.001 for IRS). Thus, odds-ratio (OR) was evaluated for 10% AR’s cut-off and the risk to develop a brain metastasis was 8,33 times higher in women with AR-negative primary EOCs (CI 95%: 2.15 - 32.29). (See Table 4)
Combined Analysis
We analyzed the combined dataset including previous published cohort and new validation cohort, for a total of 40 cases and 40 controls.
Case dataset
Median age at diagnosis was 57 years (range 39-76); 34/40 cases were categorized as serous carcinomas (85%) and all cases were considered as high grade (G3) tumors (40/40, 100%). As for FIGO classification, 4 cases (10%) were stage II, 25 (62.5%) stage III and 11 (27.5%) stage IV.
Most of our cases (31/40, 77.5%) was treated with up-front surgery; nine (22.5%) received neo-adjuvant chemotherapy (NACT) followed by Interval Debulking Surgery (IDS). Each case received a platinum-based chemotherapy, with Carboplatin alone (2/40, 5%) or in combination with paclitaxel, (38/40, 95%). Residual tumor was present in 17 cases (42.5%), absent in 14 (22.5%), unknown for 9 patients (22.5%).
All cases relapsed, with a median PFS of 18 months (range 0-62). Median age at diagnosis of CNS involvement was 59.5 years, with a median bPFS of 25 months (range 0-87 months). Twenty one out of 40 (52.5%) patients developed brain metastases as the first site of relapse. Further sites of first relapse were lymph nodes and/or peritoneum (14/40, 35%) lung or liver (5/40, 12.5%).
Overall, median bOS resulted 12 months (range 2-112), while median OS was 47.5 months (range 4-173).When statistical analyses were performed (May 2018), 10/40 patients (25%) were alive, whilst 29 (72.5%) had died; vital status datum was not available for one patient (2.5%).
Table 5 shows the most relevant clinico-pathological parameters of case subgroup.
For more details about features of CNS involving see Table 2.
Table 5 Clinico-pathological features of primary ovarian lesion of combined dataset: case dataset vs control dataset
|
Clinico-histopathological features
|
Case Dataset
n=40 (%)
|
Control Dataset
n=40 (%)
|
p Value
|
Age, median (years) [range]
|
57[39-76]
|
63.5[36-78]
|
0.960
|
Histological type
Serous
Clear cell
Endometrioid
Mucinous
Squamous
Undifferentiated
|
34 (85)
2 (5)
1 (2.5)
1 (2.5)
1 (2.5)
1 (2.5)
|
40 (100)
|
0.262
|
Histological grade
G3
|
40 (100)
|
40 (100)
|
1
|
FIGO stage
II
III
IV
|
4 (10)
25 (62.5)
11 (27.5)
|
4 (10)
25 (62.5)
11 (27.5)
|
1
|
Type of surgery
Upfront
Neoadjuvant CT + IDS
|
31 (77.5)
9 (22.5)
|
18 (45)
22 (55)
|
0.003
|
Macroscopic residual tumor
Present
Absent
|
17 (42.5)
14 (35)
|
19 (47.5)
20 (50)
|
0.611
|
Not available
|
9 (22.5)
|
1 (2.5)
|
|
First-line chemotherapy
|
|
|
|
Platinum-based
|
40 (100)
|
40 (100)
|
1
|
Relapse
Present
Absent
|
40 (100)
|
30 (75)
10 (25)
|
0.001
|
First site of relapse
CNS
Lymph nodes and / or peritoneum
Other
|
21 (52.5)
14 (35)
5(12.5)
|
28 (93.3)*
2 (6.7)*
|
<0.001
|
Patient’s status
Alive
Dead
Not available
|
10 (25)
29 (72.5)
1 (2.5)
|
21 (52.5)
19 (47.5)
|
0.015
|
PFS, median (months) [range]
|
18 [0-62]
|
17.5 [5-73]
|
|
OS, median (months) [range]
|
47.5 [4-173]
|
40 [6-101]
|
|
|
*Disease progression did not occur for 10 patients.
IDS: Interval Debulking Surgery; CT: Chemotherapy; CNS: Central Nervous System; PFS: Progression Free Survival; OS: Overall Survival.
|
Control dataset.
This group included 40 women with a median age of primary EOC diagnosis of 63.5 years (range 36-78). All of our controls were identified as high grade (G3) serous carcinomas (40/40, 100%). There were 4 FIGO stage II (10%), 25 FIGO stage III (62.5%) and 11 FIGO stage IV (27.5%). Most patients (22/40, 55%) was treated with neoadjuvant chemotherapy (Carboplatin alone, 1/22 4.5%, Carboplatin and paclitaxel, 19/22 86.4%, Carboplatin, paclitaxel and Bevacizumab, 2/22 9.1%) followed by IDS. Up-front surgery was chosen for the remaining 18 women, followed by adjuvant chemotherapy (Carboplatin plus paclitaxel, 13/18 72.2% Carboplatin, paclitaxel and Bevacizumab, 3/18 16.7%, Carboplatin and Pegylated Liposomal Doxorubicin 1/18 5.6%, Carboplatin, Pegylated Liposomal Doxorubicin and Bevacizumab, 1/18 5.6%). Nineteen patients (47.5%) had residual tumor after surgery; for one patient (1/40, 2.5%) this datum was not retrievable. Thirty out of 40 controls (75%) experienced at least one relapse of the disease, whose first localization involved either lymph nodes and/or peritoneum (28/30, 93.3%) or liver (2/30, 6.7%). Median PFS was 17.5 months (range 5-73), whereas median OS was 40 months (range 6-101).When data were processed, 19 (47.5%) patients had died.
Table 5 shows the most relevant clinico-pathological parameters of control subgroup of combined dataset.
Cases and Controls proved to be comparable populations: no statistical difference was observed for age (p=0.960), histotype (p=0.262), tumor grade (p=1), FIGO stage (p=1), residual tumor after surgery (p=0.611) and first line chemotherapy (p=1) (Table 5). There were significant differences between cases and controls, in particular upfront surgery vs interval cytoreductive surgery, incidence of relapse and number of surviving patients.
For AR protein expression of combined cohort as continuous variable of primary vs metastatic lesions and of cases vs controls see Table 6 (see below). AR expression in cases and controls dataset of combined cohort considered as dichotomized variable is showed in Table 7 (see below)
Table 6 Immune-histochemical results and statistical analyses of AR considered as continuous variable: comparisons of both cases vs controls and primary vs metastatic lesions
|
IHC parameter
|
Cases vs controls //
primary vs metastatic lesions
(%)
|
N
|
Mean
(%)
|
Median (%)
|
Range
|
p Value
|
|
|
|
|
|
|
|
AR
|
Cases
|
39
|
14.15
|
5
|
0 - 70
|
< 0.001
|
Controls
|
40
|
42.05
|
37.5
|
0 - 95
|
Primary tumor
|
24
|
12.70
|
2.5
|
0 - 70
|
0.270
|
Brain metastasis
|
24
|
9.25
|
0
|
0 - 60
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
|
AR: Androgen Receptor
|
Table 7 Immune-histochemical results and statistical analyses of AR considered as dichotomized variable as for both cases and controls datasets
|
IHC parameter
|
Cut-off
|
Case dataset (primary ovarian lesions)
(%)
|
Control dataset (primary ovarian lesions)
(%)
|
p Value
(Cases vs controls: IHC comparison)
|
OR
(Cases vs controls)
(CI 95%)
|
|
|
|
|
|
|
|
|
AR
|
< 1%
|
7/39 (17.9)
|
2/40 (5)
|
0.087
|
|
|
≥ 1%
|
32/39 (82.1)
|
38/40 (95)
|
|
|
< 10%
|
26/39 (66.7)
|
7/40 (17.5)
|
< 0.001
|
9.429 (3.290 – 27.020)
|
|
≥ 10%
|
13/39 (33.3)
|
33/40 (82.5)
|
IRS ≤ 2
|
31/39 (79.5)
|
13/40 (32.5)
|
< 0.001
|
|
|
IRS > 2
|
8/39 (20.5)
|
27/40 (67.5)
|
|
|
|
|
|
|
|
|
|
|
AR: Androgen Receptor
|
AR expression is significantly reduced in cases vs controls’ combined cohort
Case dataset vs. control dataset. AR shows a statistically significant difference between cases and controls when considered as continuous variable (mean case dataset: 14.15%; mean control dataset: 42.05%, p<0.001, Table 6).
Considered as dichotomized variable, the two populations showed different expression of AR (p<0.001 for both 10% cut-off and IRS). Thus, odds-ratio (OR) evaluated for 10% AR’s cut-off resulted 9.43 (CI 95%: 3.290 – 27.020) (See Table 7).
Figure 1 shows the immune-histochemical expression of AR with the corresponding H&E staining in two representative cases and two controls.
AR expression is not differentially expressed in primary ovarian cancers vs paired brain metastases
Primary ovarian cancers vs paired brain metastases. IHC expression of AR doesn’t exhibit statically significant difference of expression between the two groups in the combined population, considering continuous variable only (See Table 6).
Kaplan-Meier’s curves of combined population.
Survival curves were obtained using PFS (progression free survival) and bPFS (progression brain metastasis free survival) as events of interest in the combined population. AR results associated with prognosis in this population as show the Kaplan-Meier’s (KM) curves, in particular: KM curve by AR 10% and PFS (Figure 2, curve A, p=0.002) and KM curve by AR 10% and bPFS (Figure 2, curve B, p=0.005).