Document Type : Original Article
Authors
1 Clinical Oncology & Nuclear Medicine Department, Faculty of Medicine, Al-Azhar University
2 clinical oncology and nuclear medicine faculity of medicine al azhar university
3 Therapeutic Radiology and Nuclear Medicine, Al-Azhar University
Abstract
Keywords
INTRODUCTION
Worldwide, prostate cancer is the second most common cancer and the fifth leading cause of death from cancer in men, with an estimated 164.690 new case diagnosed in 2018 at united states, mortality rate from prostate cancer is also estimated to be about 9% of male cancer death in 2018. 1
About 4% of prostate cancer patients presented with metastatic disease on initial diagnosis, and about one-third of localized prostate cancer patients experience disease progression during the course of treatment. 2
Most of prostate cancers that diagnosed with localized disease are considered less aggressive malignancy because of their indolent course; nonetheless, metastatic prostate cancer is still lethal. The 5-year survival rate approaches 100% for low risk patients with localized disease, but once the metastases occurs the disease become practically incurable and 5 years survival declined to 28%. 3
Since the usage of prostate-specific antigen (PSA) tests increased as screening purpose, early detection of prostate cancer has increased, and death from prostate cancer has been gradually reduced over time. However, the concerns about the over diagnosis and over treatment have increased. As a result, in 2008 and 2012 United States Prevention Services Task Force (USPSTF) recommended against routine PSA screening. After this, a decline in the incidence of localized prostate cancer has been reported, and these have been a raising concern for worsening of prostate cancer-specific survival. Based on some recent studies, intermediate- or high-risk prostate cancer reported to increase by 6% from 2011 to 2013, which support this concern. In addition, metastatic prostate cancer has been increased from 2004 to 2013.4,5
Androgen suppression using bilateral orchiectomy or luteinizing hormone releasing hormone (LHRH) agonist/antagonist should be first-line treatment along with short-course anti-androgen to prevent disease flare at starting treatment with LHRH.6
Androgen Deprivation Therapy (ADT) is associated with a wide range of side effects that can significantly impair quality of life, Important and/or frequent side effects include loss of lean body mass, increased body fat, decreased muscle strength, decrease bone mineral density and sexual dysfunction.7 The treatment of metastatic cancer prostate has significantly changed over the past 5 years. Since 2015, two clinical trials, CHAARTED and STAMPEDE arm C, demonstrated that up-front docetaxel plus ADT improves overall survival (OS).8,9
Then, in 2017, two clinical trials, LATITUDE and STAMPEDE arm G, showed that up-front abiraterone plus prednisone plus ADT improves OS to a similar degree as docetaxel plus ADT did.10,11
MATERIAL AND METHODS
This retrospective study included all patients diagnosed with metastatic prostate cancer, registered and treated at our clinical Oncology Department, Al-Hussein University hospital in the period between January 2007 and December 2016. Charts of included patients had been reviewed and relevant data were collected and statistically analyzed.
The study Included male patient regardless of age who have had pathologically proven prostate cancer, radiological documented distant metastasis and performance status ranging from 0-III WHO; on the other hand patients who have secondary malignancy, performance status IV or received any kind of treatment outside our facility were excluded from the study.
The relevant data collected in the study included; patient related data (age, sex, family history and comorbidity); disease related data (baseline and follow-up PSA, Gleason score, tumor grade, number of biopsied cores, number of positive cores, percentage of positive disease in each core and finally, local and systemic extent of the disease); and treatment related data including type, toxicity, response and progression free survival related to each line of therapy.
Patients were classified based on metastasis load into two categories; high volume disease and low volume disease according to presence or absence of visceral metastasis and, sit and number of bone lesions, as following; high volume disease defined as the presence of visceral metastases or at least four bone lesions with one or more beyond the vertebral bodies and pelvis and low volume disease include those who had no visceral metastasis and less than three sites of bone metastasis.
Data were coded and entered using the statistical package SPSS version 23. Data was summarized using mean, standard deviation, median, minimum and maximum for quantitative variables and frequencies (number of cases) and relative frequencies (percentages) for categorical variables. Survival interval conspired as time between the date of histological diagnosis and the date of the last follow-up (for censored observations) or the date of death (for uncensored observations), while progression free interval was considered as time between date of the first treatment and the date of the last follow-up (for censored observations) or; date of death or disease progression whichever happen first (for uncensored observations). One-sided log-rank of Kaplan—Meier survival estimates was used for statistical analysis of overall survival and progression free survival, while the unpaired T test and one-way ANOVA test were used in the univariate analysis of the variables. Results of P-value less than 0.05 were considered statistically significant.
ETHICAL APPROVAL:
The current investigation had been approved by the ethical committee, Faculty of Medicine, Al-Azhar University, Cairo, Egypt, before the start of this study.
RESULTS
After reviewing the charts of 100 patients who reported to have prostate cancer in our archive, 39 patients was found to have metastatic prostate cancer (illegible for the study), among these illegible patients; mean age was 66.1 years (range 51:78 ); 19 patients (47.4%) were cigarette smoker and 20 patients (52.6%) were non-smokers; family history of malignancy was reported by 14 patients (34.2%); most of the patients was presented with WHO performance status (PS) II, 18 patients (47.4 %), while 11 patients (26.4%), and 10 patients (26.3%) were having PS 0-I and PS III-IV respectively; the most common presenting symptoms were urination-related symptoms in 24 patients (61.6%) followed by boney aches in 15 patients (38.4.8%). (Table 1)
All patients were having prostate adenocarcinoma on TRUS core needle biopsy, the median number of biopsied cores was 6 (range 6 : 12), while the median number of positive cores was 4 (range 3- 8), median percentage of malignancy in each cores was 70% (range 25 :100 ); Gleason score (GS) ≤ 6 was reported in four patients (7.9%), while GS 7 and GS 8-10 were reported in 15 patients (39.5%) and 20 patients (52.6%) respectively; all patients were having bone metastasis, of them 30 patients (76.3%) had high volume disease and 9 patients (23.7 %) had low volume disease, while 15 patients (38.3 %) was having visceral metastasis, median baseline PSA level was 70 ng/ml (range 10:1850). (Table 1)
Bilateral orchiectomy was first line treatment in 21 patients (52.6 % ), while 18 patients (47.4%) received ADT as primary treatment, in 14 patients (33.8%) ADT was LHRH agonist + bicultamide and LHRH agonist + flutamide acetate in four patient (22.2%); biochemical response to primary hormonal treatment was reported in 70% of patients; the most noticed treatment related toxicity were mild anemia in 7 patients and osteoporosis in 4 patients while grade 3-4 toxicity was not reported. (Table 2,3)
palliative radiotherapy was used at presentation in 8 patients who presented to us with cord compression , with subjective improvement in lower limb weakness and motor power, while used during later time in 30 patients who developed bone pain as palliative treatment of pain and tenderness and in one patient with brain metastasis, Second line hormonal treatment in 21 patients (52.6%) as following, 9 patients (22.5%) received LHRH agonist gasroline acetate + bicultamide,10 patients (25% ) received flutamide, one patient (2.5%) received surgical casterization + biclutamide and 1patient (2.5%) received biclutamide with doubled dosage , With biochemical response in (57%) of patients while chemotherapy was used as in 6 patients (15%) in form of Docetaxel from six to ten cycles with reported toxicity neutropenia in halve of cases and fatigue, biochemical response was noticed in (50%) of patients. (Table 4)
|
|
No. |
(%) |
|
Age |
||
|
Mean ± SD |
66.1±8.4 |
|
|
Minimum |
51 |
|
|
Maximum |
78 |
|
|
Grade |
||
|
2 |
14 |
28.9% |
|
3 |
25 |
63.2% |
|
Family history (positive) |
14 |
34.2% |
|
Smoking (Positive) |
19 |
47.4% |
|
Co- morbidities |
||
|
DM (positive) |
12 |
31.6% |
|
HTN (positive) |
20 |
52.6% |
|
Performance status ECOG score |
||
|
0-1 |
11 |
26.4% |
|
2 |
18 |
47.4% |
|
3 |
10 |
26.3% |
|
|
|
|
|
Presentation |
||
|
Prostatism |
19 |
50% |
|
Bony aches |
15 |
44.8% |
|
Hematouria |
3 |
5.3% |
|
Less than70 PSA |
19 |
47.4% |
|
More than 70 PSA |
20 |
52.6% |
|
Site of metastasis |
||
|
low volume bone metastasis |
9 |
23.7% |
|
High volume bone metastasis |
30 |
76.3% |
|
Visceral mets |
15 |
38.3 |
|
First line treatment |
|
|
|
Medical Hormonal treatment |
18 |
47.4% |
|
Surgical Hormonal treatment |
21 |
52.6% |
|
Gleason score |
||
|
≤ 6 |
4 |
7.9 |
|
7 |
15 |
39.5 |
|
8-10 |
20 |
52.6 |
Table 1: Patient characteristics
|
|
Frequency |
Percentage% |
|
Surgical castration |
21 |
52.6% |
|
ADT alone |
18 |
47.4% |
Table 2 :First line management
|
|
Total no (39) |
% |
|
|
First line hormonal |
Biclutamide + Goserline acetate |
14 |
33.8% |
|
Flutamide + Goserline acetate |
4 |
10.2% |
|
|
Surgical/l castration |
21 |
53.8% |
|
Table 3 : Type of Hormonal treatment in 1st line
|
Palliative radiotherapy (n = 39) |
No Rth received |
10 |
25.3% |
|
Bone mets |
28 |
73.7% |
|
|
Brain mets |
1 |
1 |
Table 4 : Palliative radiotherapy
After a median follow up period four years, median PFS was (18.4) months and one year PFS was reported in about (70%) of patients after 1st line hormonal treatment. (Figure 1)
Fig. 1: Represent the progression free survival in all eligible cases
Median OS was (25.5) range months and 1year OS was reported in( 83 %) Of studied cases. (Figure 2)
Fig. 2: Represent the overall survival in all eligible cases
several factors that could affect metastatic patients who received hormonal treatment had been studied in relation to both PFS and OS . only two factors had significant impact on overall survival; performance status and PSA value at presentation. (Figure 3) (Table 5,6)
Fig. 3: Represent effect of PSA on overall survival in all eligible cases
|
All parameters |
No. (39) |
Median |
C.I. 95% |
P-value |
|||||||
|
Lower |
Upper |
||||||||||
|
Age (years) |
≤68 |
21 |
31.1 |
33.8 |
38.3 |
0.256 |
|||||
|
>68 |
18 |
21.0 |
19.7 |
22.2 |
|||||||
|
Smoking |
No |
19 |
25.5 |
21.8 |
29.2 |
0.079 |
|||||
|
Yes |
20 |
34.3 |
17.8 |
50.6 |
|||||||
|
Performance |
0. I |
11 |
37 |
31.53 |
42.47 |
0.05 (S) |
|||||
|
II |
18 |
24 |
17.56 |
30.44 |
|||||||
|
III |
10 |
18.1 |
16.7 |
19.4 |
|||||||
|
DM |
No |
27 |
21.0 |
18.8 |
23.8 |
0.161 |
|||||
|
Yes |
12 |
31.0 |
22.5 |
39.3 |
|||||||
|
HTN |
No |
17 |
25.5 |
18.3 |
32.6 |
0.629 |
|||||
|
Yes |
22 |
29.2 |
18.2 |
40.3 |
|||||||
|
Gleason score |
7 |
3 |
38.9 |
000 |
38.9 |
0.951 |
|||||
|
6 |
17 |
29.3 |
22.8) |
35.9 |
|||||||
|
7 |
19 |
21.0 |
(19.6 |
22.3 |
|||||||
|
Bone scan |
Low |
9 |
25.5 |
000 |
25.5 |
0.780 |
|||||
|
High |
30 |
24.5 |
16.2 |
32.8 |
|||||||
|
Bone modifying agents |
Free |
25 |
24.5 |
19.4 |
29.6 |
0.926 |
|||||
|
Zolidronic acid |
14 |
29.2 |
12.9 |
45.6 |
|||||||
|
Grade |
II |
14 |
29.3 |
22.4 |
36.1 |
0.976 |
|
||||
|
III |
25 |
21.0 |
18.9 |
23.1 |
|
||||||
|
PSA |
≤70 |
19 |
22.3 |
16.6 |
11.1 |
0.052 |
|
||||
|
>70 |
20 |
11.0 |
10.9 |
38.0 |
|
||||||
|
Positivity |
≤50 |
19 |
25.5 |
16.9 |
34.0 |
0.786 |
|
||||
|
>50 |
20 |
22.0 |
15.9 |
16.0 |
|
||||||
|
Casterization |
Surgical |
21 |
29.3 |
23.6 |
34.8 |
0.140 |
|
||||
|
Treatment |
18 |
22.0 |
17.7 |
24.3 |
|
||||||
Table 5: Correlation between overall survival with different factors
|
All parameters |
No. (39) |
Median |
C.I. 95% |
P-value |
||
|
Lower |
Upper |
|||||
|
Age (years) |
≤68 |
21 |
18.9 |
15.1 |
22.8 |
0.710 |
|
>68 |
18 |
18.1 |
16.2 |
19.9 |
||
|
Smoking |
No |
19 |
20.1 |
16.3 |
23.8 |
0.205 |
|
Yes |
20 |
16.2 |
14.2 |
18.1 |
||
|
Performance |
0. I |
11 |
18 |
0.76 |
16.52 |
0.302 |
|
II |
18 |
16 |
2.27 |
11.56 |
||
|
III |
10 |
6 |
4.00 |
0.00 |
||
|
DM |
No |
27 |
18.1 |
16.5 |
19.6 |
0.288 |
|
Yes |
12 |
19.2 |
16.1 |
22.3 |
||
|
HTN |
No |
17 |
18.9 |
17.1 |
20.8 |
0.255 |
|
Yes |
22 |
18.1 |
16.0 |
20.1 |
||
|
Gleason score |
7 |
3 |
18.9 |
000 |
18.9 |
0.951 |
|
6 |
17 |
22.4 |
18.4 |
24.4 |
||
|
7 |
19 |
18.1 |
17.2 |
18.9 |
||
|
Bone scan |
low |
9 |
22.5 |
20.0 |
24.9 |
0.233 |
|
High |
30 |
18.1 |
16.7 |
19.4 |
||
|
Bone modifying agents |
Free |
25 |
18.1 |
16.9 |
24.9 |
0.823 |
|
Zometa |
14 |
18.9 |
14.4 |
23.4 |
||
Table 6: Correlation between PFS and different patient characteristics
DISCUSSION
Prostate cancer account for 2.5 % of all cancers presented to our department from the period between January 2007 and December 2016 Our study is not consistent with the published data in our country according to the results of the National Population-Based Cancer Registry Program (NCRP) In Egypt, prostate cancer is the 6th most common male cancer it comprised 4.7% of malignancies in males.12
Treatment options include active surveillance, surgery (open, laparoscopic, or robotic-assisted), external beam radiation, or brachy therapy. Hormonal therapy may be used along with surgery or radiation therapy in more advanced cases. More advanced disease is treated with hormonal therapy, chemotherapy, radiation therapy, and/or other treatments.13
In our retrospective study, we examined individual and clinico-epidemiological factors contributing to overall PCa survival, PFS in prostate cancer patients at the archive of Clinical Oncology and Nuclear Medicine Department, Al-Hussein Hospital, Al-Azhar University.
The study population number was 39 male patients. The mean age of the studied population was 66 years (range 51:78) consistent with mean age worldwide which is 67 years.14
In our study OS was statistically insignificant with age although patients
Much co-morbidity were associated with prostate cancer seen in higher age population. Most of the patients were older than 65 years old. In our study, the most relevant co-morbidity among studied population was cardiovascular disease in which 52.6%of the patients complaining of hypertension and 7.9% had IHD. Diabetes mellitus (DM) was found in 31.6% of patients.
Similarly, Spanish data reported that of all co-morbidities 48.15% of the patients complained of cardiovascular diseases and 14.41% complained of Diabetes mellitus. Much co-morbidity were associated with prostate cancer seen in higher age population.15
In the United States, most prostate cancers patients are diagnosed because of screening; they are mostly asymptomatic at time of diagnosis. With a small percentage having local symptoms, which usually indicates locally advanced disease. While, in our study, most of patients presented with variable symptoms; the most common was prostatism in 61.6% of patients including irritative and obstructive urinary symptoms and bony aches in 38.8%. The lack of awareness and absence of a screening program led to the late presentation of most our patients16.
They found that among the 6,457 men diagnosed with prostate cancer in Florida during 2001– 2007, about 12.70% were diagnosed with advanced stage of prostate cancer. While in our study 54% of patients had local disease and 46% had distant stage. The lack of awareness and the late presentation of the patient consistent with the fact that the study population from a single tertiary referral unit are the reasons of our results and likely due to absence of co-operation between us and urological department so they accept patients with localized prostate cancer that will underwent surgery and keep patients under follow up and refer them to us when become metastatic so this justify high percentage of metastatic patients.16
In our study patients treated with ADT demonstrated that defined LV patients had a longer overall survival (25.5months) and progression free survival (22.5 months) compared to patients with HV disease OS (24.5 months) and PFS (18.1 months) which are consistent with those of the post-hoc analysis of the CHAARTED trial and of the CHAARTED-GETUG-AFU15 combined study.16
Worldwide Median OS was 42.1 months and median failure-free survival was 11.2 months and the superiority of their results as a result regular follow up to patients under study.17
While In our study, initially metastatic prostate cancer patients had median overall survival of 25.5 months (95% CI 20.3-30.6) and the median PFS was found to be 18.4 months (95% CI 16.8-19. 9) which was statistically insignificant. Our results could be explained by the heterogeneous population in our study and the lack of regular follow up by our patients. This may due to lack of new line of treatment that not financially supported from ministry of health which make us in circle of traditional line of treatment which may reflect a much better survival estimated in western countries.
In our study ADT either medical or surgical casterization was the first line treatment. Patients subjected to surgical casterization by bilateral orchiectomy or received hormonal treatment by luteinizing hormone–releasing hormone (LHRH) agonists such as gosereline and anti-androgen such as biclutamide or flutamide which similar to data published.18
After progression another line of hormonal treatment was used either surgical casterizatin or medically by anti-androgens or increasing the dose of anti-androgen. In patients whose sill developing progression chemotherapy used and only 6 patients (15%) received dosetaxel from 6 to 10 cycles with PFS 6 months range from (3 -11) months which similar to data published TAX 327 study by.19
But Recently, Chaarted and Stampede studies demonstrated a survival benefit for men with metastatic hormone-sensitive PC (mHSPC) treated with docetaxel plus ADT as first line. Results of the CHAARTED trial were presented in 2014 and published in 2015. Median OS was significantly improved in the ADT plus D arm (57.6 vs 44.0 ms; HR: 0.61; p < 0.001). 8,9
In order to account for limitations, other than the inherent retrospective nature of the current study, a relatively short follow-up exists considering the long natural history of prostate cancer and lack of usage of the current trends in therapy are evident. However, it remains a viable report of management of this disease even if at a single institutional level.
CONCLUSION
Outcome of metastatic prostate cancer patients who have been treated at our center significantly affected by PS at presentation and baseline PSA level, however the absolute survival number needs to be improved by implementation of newly approved drugs in the 1st and 2nd lines, that isn’t currently available in our center.
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