The Potential Clinical and Economic Value of Primary Tumour Identification in Metastatic Cancer of Unknown Primary Tumour: A Population-Based Retrospective Matched Cohort Study.

PURPOSE: Several genomic tests have recently been developed to identify the primary tumour in cancer of unknown primary tumour (CUP). However, the value of identifying the primary tumour in clinical practice for CUP patients remains questionable and difficult to prove in randomized trials.
OBJECTIVE: We aimed to assess the clinical and economic value of primary tumour identification in CUP using a retrospective matched cohort study.
METHODS: We used the Manitoba Cancer Registry to identify all patients initially diagnosed with metastatic cancer between 2002 and 2011. We defined patients as having CUP if their primary tumour was found 6 months or more after initial diagnosis or never found during the course of disease. Otherwise, we considered patients to have metastatic cancer from a known primary tumour (CKP). We linked all patients with Manitoba Health databases to estimate their direct healthcare costs using a phase-of-care approach. We used the propensity score matching technique to match each CUP patient with a CKP patient on clinicopathologic characteristics. We compared treatment patterns, overall survival (OS) and phase-specific healthcare costs between the two patient groups and assessed association with OS using Cox regression adjustment.
RESULTS: Of 5839 patients diagnosed with metastatic cancer, 395 had CUP (6.8%); 1:1 matching created a matched group of 395 CKP patients. CUP patients were less likely to receive surgery, radiation, hormonal and targeted therapy and more likely to receive cytotoxic empiric chemotherapeutic agents. Having CUP was associated with reduced OS (hazard ratio [HR] 1.31; 95% confidence interval 1.1-1.58), but this lost statistical significance with adjustment for treatment differences. CUP patients had a significant increase in the mean net cost of initial diagnostic workup before diagnosis and a significant reduction in the mean net cost of continuing cancer care.
CONCLUSION: Identifying the primary tumour in CUP patients might enable the use of more effective therapies, improve OS and allow more efficient allocation of healthcare resources.

Key Points for Decision Makers

Introduction

Approximately 15% of all new cancers present with metastases at time of diagnosis [1]. Primary site determination for metastatic cancers is the starting point to define standard-of-care patient management. In approximately two-thirds of these cases, the primary tumour becomes apparent early during the course of the initial diagnostic workup [2]. The remaining metastatic cancers represent challenging cases as tumours of uncertain primary origin. For these cases, pathologists and oncologists often undertake a comprehensive diagnostic workup that may include cytogenetic studies, electron microscopy, endoscopies and immunohistochemical (IHC) analysis [2, 3]. Although clinical and pathologic investigations are recommended to be sign and symptom guided [2, 3], they often require a longer hospital stay accompanied by painful and distressing investigations and may incur increased costs for the healthcare system [4, 5]. However, a primary tumour site is identified in <30% of these cases [6, 7]. Consequently, over 6800 cases with histologically proven metastatic cancer of unknown primary origin (CUP) are diagnosed annually in Canada despite diagnostic assessment.

Although it is accepted that CUP is a heterogeneous collection of metastatic malignancies [6], there is no consensus on whether CUP is simply a group of metastatic tumours with undetected primary tumours or a distinct entity with specific genetic characteristics [6]. Clinically occult primary tumours have subsequently been anatomically detected at autopsy in about 75% of CUP patients [8]. In addition, approximately 7% of CUP patients have their latent primary (LP) tumour clinically detected months to years after initial diagnosis [9]. Most metastatic tumour biopsies from CUP patients are completely undifferentiated or poorly differentiated, with the majority being adenocarcinomas, but other histologies have also been diagnosed (e.g. lymphoma, melanoma, sarcoma) [1, 10].

In the absence of a specific primary tumour diagnosis, treatment guidelines vary [3]. When appropriate, CUP patients are typically treated with empirical cytotoxic chemotherapy regimens [11, 12]. Despite this, CUP patients have a poor prognosis, with median survival typically ranging from 7 to 11 months [6].

In recent years, the emergence of gene expression tumour-profiling assays (messenger RNA [mRNA] or microRNA platforms) as adjuncts to current clinicopathologic evaluations has offered the potential to correctly identify the primary tumour in about 90% of patients with CUP [7, 13–26]. This breakthrough, coupled to the recent emergence of targeted drugs for patients with known primary tumour (CKP) fuelled hopes for a revamp of CUP management [27-29]. Although the clinicopathologic presentation of CUP patients may differ from that of patients with CKP, there does not seem to be a major disparity in the response rates and the outcomes between these two patient groups after the primary tumour is defined and tumour-specific therapies are administered [29]. However, the impact of primary tumour identification via gene expression profiling on clinical outcomes for patients with CUP remains uncertain and difficult to prove in randomized trials because of a combination of ethical, clinical and logistical considerations [29-31]. Additional clinical evidence is necessary to optimize a precision medicine strategy as a standard of care for patients with CUP. In addition, the impact of primary tumour identification on the cost of care throughout the course of metastatic disease will be an important element in the formulation of new provincial guidelines and reimbursement policies for CUP management and necessary to inform healthcare resource allocation and fiscal planning for the prospective precision medicine era of care for CUP.

In this study, we aimed to estimate the potential clinical and economic value of primary tumour identification in CUP using heath administrative databases from the Canadian province of Manitoba to carry out a propensity score matched-cohort analysis in which we evaluated differences in clinical and economic outcomes between patients with CUP and their matched counterparts with CKP.

Patients and Methods

Data Sources and Identification of Study Population

The Manitoba Cancer Registry (MCR) and Provincial Pharmacy program at CancerCare Manitoba (CCMB) and Manitoba administrative databases held by Manitoba Health, including the Hospital Discharge Database, Physician Claims Database and the Drug Program Information Network (DPIN), served as the data sources for this analysis. A full description of these databases and their contents has been reported elsewhere [30-33].

We have previously used the MCR to identify a cohort of patients diagnosed initially with metastatic cancer during the period from 1 January 2002 to 31 December 2011 [34] and identify when these patients had their primary tumour diagnosed during the course of their disease. The cohort was limited to Manitoba residents who had undergone clinical and pathological diagnostic evaluation in Manitoba and with no history of other malignancy at initial diagnosis. A minimum of 2-year follow-up information from the time of initial diagnosis was available for each patient. Follow-up information included diagnosis of second primary, cancer treatments (e.g. surgical and therapeutic radiology procedures, systemic therapy and palliative care) and death. Full details regarding the identification of this metastatic patient population and the process by which we identified when primary tumours were diagnosed are reported elsewhere [34].

For this analysis, we used this metastatic patient population to identify all patients who had their metastatic disease histologically confirmed and survived at least 6 months following their initial cancer diagnosis. This 6-month window was used to ensure that patients would have had reasonable time during the early course of their metastatic disease to undergo all necessary clinical and pathological diagnostic evaluations (i.e. diagnostic workup) and had their primary tumour sites diagnosed [9]. We stratified patients by their primary tumour diagnostic status (CUP vs. CKP). We defined patients as having CUP if their primary tumour was initially unidentified (i.e. International Classification of Diseases for Oncology [ICD-O] code C80.9) and either had their LP tumour diagnosed at least 6 months after their initial diagnosis or who never had their LP tumour diagnosed during the 2-year follow-up period. The 6-month window was used to ensure the identification of the LP tumour was not the result of extension in the initial diagnostic workup and is considered conservative compared with other attempts at identifying CUP using a 2-month window [9]. We defined patients as having CKP if their primary tumour was initially identified during the 6 months after their initial diagnosis and no change was detected in their primary tumour diagnostic status later during the 2-year follow-up period.

Linkage with the Provincial Pharmacy Program Database at CCMB and Manitoba Administrative Databases

We linked the two patient groups with the Provincial Pharmacy Program of CCMB and Manitoba Health’s administrative databases to validate all cancer therapy data captured by the MCR; to collect additional information on types of radiotherapy and systematic therapy agents; to measure co-morbidity; and to estimate direct healthcare costs. To protect confidentiality, the linkage was performed with a scrambled unique health number using anonymized versions of these databases. Records of these databases for each patient in the study cohort were available between 3 years before and 2 years after initial cancer diagnosis.

Comorbidity Index

We determined co-morbidity from the Hospital Discharge Database and the Physician Claims Database through diagnoses that were recorded for each patient in the study cohort during all patient hospital stays and physician claims between 3 years before and 6 months after initial cancer diagnosis. We used co-morbid diagnoses coded using the Charlson Co-morbidity Index, excluding cancer diagnoses, which has been used elsewhere [32-34].

We also used the Physician Claims Database to collect information on diagnostic tests and procedures undertaken during the diagnostic workup (defined as the period from 6 months before to 6 months after initial cancer diagnosis) for all identified patients diagnosed with metastatic cancer. The diagnostic tests and procedures recorded in the Physician Claims Database include the following: endoscopies, diagnostic ultrasound scans, X-rays, computerized axial tomography (CT) scans, magnetic resonance imaging (MRI) scans, diagnostic isotope procedures, fine and core needle biopsies, pulmonary function tests, lumbar puncture (spinal tap), dermatoscopy, guaiac faecal occult blood test, gynaecological physical examination, Papanicolaou (Pap) test, and dilatation and curettage.

Direct Healthcare Costs

The direct costs of healthcare services comprised inpatient and 1-day procedure stays, physician and other healthcare provider services, prescription drugs and intravenous oncology drugs. The costs of these services and drugs are all publicly funded in Manitoba and recorded in the Hospital Discharge Database [35, 36], Physician Claims Database, DPIN database and Provincial Pharmacy Program of CCMB database. We determined the healthcare costs from all records of these databases for each patient in the study cohort between 3 years before and 2 years after initial cancer diagnosis. All costs are expressed in Canadian dollars (CAD), year 2016 values, using the Bank of Canada inflation calculator [37].

We estimated the costs of various service and drug categories using a phase-of-care approach [38-41]. Costs of care for patients in the cohort were divided into five clinically relevant phases of care: (1) usual care before the onset of signs of illness; (2) initial diagnostic workup before diagnosis; (3) continuing diagnostic workup after diagnosis and initial cancer care; (4) continuing cancer care; (5) last 6 months of life. The “usual care before the onset of signs of illness” phase consisted of the time between 3 years and 6 months before diagnosis. We defined the “initial diagnostic workup before diagnosis” phase as the 6 months before diagnosis and the “continuing diagnostic workup after diagnosis and initial cancer care” phase as the 6 months after diagnosis. Among the patients who died, the “last 6 months of life” phase was defined as the final 6 months of life. The “continuing cancer care” phase consisted of the time between the “continuing diagnostic workup after diagnosis and initial cancer care” and “last 6 months of life” phases. Because all patients included in our study cohort survived at least 6 months following their initial cancer diagnosis (i.e. by our inclusion criteria), we first allocated costs to the first two phases of care (“usual care before the onset of signs of illness” and “initial diagnostic workup before diagnosis) and the “last 6 months of life” phase. Then, we allocated costs to the “continuing diagnostic workup after diagnosis and initial cancer care” phase, and any remaining costs were allocated to the “continuing cancer care” phase. To determine whether costs incurred during the last 6 months of the 2-year follow-up period should be allocated to the “last 6 months of life” phase or to the “continuing cancer care” phase, it was necessary to collect from the MCR an additional 6 months of death information following the 2-year follow-up from the time of initial diagnosis.

Statistical Analysis

In our primary analysis, we used the propensity score-matching method to build comparable CUP and CKP groups in terms of observable characteristics [42-44]. Full details on propensity score matching are provided as Electronic Supplementary Material (ESM).

We constructed 2-year Kaplan–Meier curves to examine the cumulative probability of overall survival (OS) for the two patient groups. The curves were compared using the log-rank test statistic. We then used a Cox proportional hazards model to test the effect of the diagnostic status of primary tumour (CUP vs. CKP) on the 2-year OS by calculating the hazard ratio (HR) for death with associated 95% confidence intervals (CIs) for CUP versus CKP. Receipt of cancer treatments (surgery [yes vs. no], radiotherapy [yes vs. no], systematic therapy [yes vs. no]), time to receive cancer treatments following initial diagnosis (number of months to surgery, radiotherapy and chemotherapy), receipt of biological targeted therapy (targeted biological therapy + chemotherapy vs. chemotherapy alone) were all tested for associations with OS and tested for their effect on the calculated HR for CUP versus CKP by adjusting the Cox proportional hazards model for these treatment covariates. We also examined whether the association of these treatment covariates with OS differed in CUP versus CKP by testing for interactions between treatment covariates and the diagnostic status of primary tumour (CUP vs. CKP).

In secondary analyses, we used three different methods to adjust for differences in baseline characteristics between the CUP group and all patients with CKP in the full cohort and examined the effect of diagnostic status of primary tumour (CUP vs. CKP) on the 2-year OS by calculating adjusted HRs and 95% CIs for CUP versus CKP. First, we adjusted for the propensity score by including it as a continuous covariate in a Cox proportional hazards model. Second, we adjusted for all baseline characteristics by including them as covariates in a traditional multivariable-adjusted Cox proportional hazards model. Third, we used a weighted Cox proportional hazards model, where the weight assigned for each patient was based on the stabilized inverse propensity score, as described elsewhere [43].

Within each phase of care and for each cost category, we calculated the cost per day for each patient in our cohort and the average cost per day separately for the CUP group, matched CKP group and all patients with CKP in the full cohort. We then estimated the average net cost per day for each phase of care following the “usual care before the onset of signs of illness” phase as the difference in average cost per day between the “usual care before the onset of signs of illness” phase and each of the following phases of care. We estimated the average net cost of an entire phase of care as the average net cost per day multiplied by the average number of days spent in that phase of care. We also calculated these cost estimates for the overall healthcare utilization by combining all cost categories.

Results

We identified 5839 patients who were initially diagnosed with metastatic cancer during the period from 1 January 2002 to 31 December 2011 and met our study inclusion criteria. Of those, 395 had CUP (6.8%) and 5444 (93.2%) had CKP (Table 1). Among those patients with CUP, 219 were women and 176 were men, accounting for 8.8% of all women and 5.3% of all men diagnosed with metastatic cancer, respectively (mean difference 3.5%, 95% CI 2.2–4.9; p < 0.0001; Table 1). Among those patients with CUP, 169 (42.8%) had their LP tumour diagnosed later, after 6 months from their initial diagnosis, and 226 (57.2%) never had their LP tumour diagnosed during the 2-year follow-up period. Table 2 shows the final classification of primary tumour site later in the course of metastatic disease for 395 patients initially diagnosed with CUP.

Table 1

Primary tumour site of 5839 patients diagnosed with metastatic cancer by sex

Primary tumour sites	Men (n = 3344)	Women (n = 2495)	All (n = 5839)
Gastrointestinal tumours	960 (28.7)	613 (24.6)	1573 (27)
Lung and pleural tumours	598 (17.9)	603 (24.2)	1201 (20.6)
Male genital system	676 (20.2)	–	676 (11.6)
Lymphoma tumours	264 (7.9)	211 (8.5)	475 (8.1)
Unknown primary tumour site	176 (5.3)	219 (8.8)	395 (6.8)
Head and neck tumours	282 (8.4)	90 (3.6)	372 (6.4)
Urological tumours	248 (7.4)	92 (3.7)	340 (5.8)
Breast tumours	1 (< 0.1)	281 (11.3)	282 (4.8)
Gynaecologic tumours	–	265 (10.6)	265 (4.5)
Melanoma (skin) tumours	60 (1)	26 (1)	86 (1.5)
Endocrine tumours	38 (1.1)	44 (1.8)	82 (1.4)
Bone and soft tissue sarcoma tumours	35 (1)	41 (1.6)	76 (1.3)
Other known primary tumours	6 (0.2)	10 (0.4)	16 (0.3)

Data are presented as n (%)

Table 2

Final classification of primary tumour later in the course of metastatic disease for 395 patients initially diagnosed with cancer of unknown primary tumour

Initial classification of primary tumour site early in the course of metastatic disease	Final classification of primary tumour site later in the course of metastatic disease	Patients, n (%)
Unknown primary tumour (n = 395)	Unknown primary tumour	226 (57.2)
	Ovary	23 (5.8)
	Colon and rectum	22 (5.5)
	Non-small cell lung	22 (5.5)
	Non-Hodgkin’s lymphoma	19 (4.8)
	Buccal cavity and pharynx	14 (3.5)
	Pancreas	12 (3)
	Bone and soft tissue sarcoma	11 (2.8)
	Stomach, small intestine, hepatocellular liver, and other digestive system	9 (2.3)
	Melanoma (skin)	7 (1.8)
	Prostate and testicular germ cell	7 (1.8)
	Kidney, renal pelvis and ureter	6 (1.5)
	Small cell lung and other lung	6 (1.5)
	Thyroid and other endocrine system	4 (1)
	Breast	3 (0.75)
	Other female genital system	3 (0.75)
	Other ill-defined sites	1 (0.25)

Prior to matching, patients with CUP presented with clinicopathological features distinct from those of their counterparts of all patients with CKP (Table 3). Using 1:1 matching on the estimated propensity score, we matched the CUP group of 395 patients with a CKP group of 395 patients. No CUP cases were dropped due to poor match quality. Table 3 shows the baseline patient and tumour characteristics of the matched CKP group as compared with the CUP group. As a result of matching, we eliminated differences between the two groups in age, sex, year of initial diagnosis, co-morbidity score, grade differentiation, histology and number and type of metastatic sites (Table 3).

Table 3

Baseline patient and tumour characteristics of 5839 patients diagnosed with metastatic cancer by diagnostic status of their primary tumours

Characteristic	Patients with CUP (n = 395)	Patients with CKP (n = 5444)	p valuea	Matched patients with CKP (n = 395)b	p valuec
Age at initial diagnosis, years	65.3 ± 13.9 (24–96)	64.3 ± 13.1 (19–103)	0.14	65 ± 13.9 (20–100)	0.9
Year of initial diagnosis
2002–2003	85 (21.5)	949 (17.4)	0.06	84 (21.3)	0.9
2004–2005	75 (19)	1225 (22.5)		71 (18)
2006–2007	85 (21.5)	1185 (21.8)		84 (21.3)
2008–2009	91 (23)	1104 (20.3)		94 (23.8)
2010–2011	59 (15)	981 (18)		62 (15.7)
Sex
Men	176 (44.6)	3168 (58.2)	<0.0001	175 (44.4)	0.9
Women	219 (55.4)	2276 (41.8)		220 (55.6)
Grade differentiation or cell indicator
Well differentiated	7 (1.8)	170 (5)	<0.0001	9 (2.2)	0.9
Moderately differentiated	20 (5)	1259 (37.2)		21 (5.3)
Poorly differentiated	65 (16.5)	1448 (42.7)		63 (15.9)
Undifferentiated	286 (72.4)	2209 (40.6)		287 (72.6)
T cell/B cell	17 (4.3)	358 (6.6)		15 (3.8)
Histology
Adenocarcinomas	157 (39.7)	2645 (48.6)	<0.0001	157 (39.7)	0.9
Squamous cell carcinoma	49 (12.4)	557 (10.2)		51 (12.9)
Mucinous and serous	26 (6.6)	235 (4.3)		27 (6.8)
Undifferentiated carcinoma	114 (28.8)	895 (16.4)		112 (28.3)
Melanoma	11 (2.8)	96 (1.8)		10 (2.5)
Complex mixed and stromal	5 (1.3)	24 (0.4)		6 (1.5)
Transitional cell, ductal lobular medullary, complex epithelial, soft tissue sarcomas, myomatous, germ cell, miscellaneous bone, nerve sheath	14 (3.5)	473 (8.7)		13 (3.3)
Hodgkin’s lymphoma, NHLs, other lymphoma	19 (4.8)	475 (8.7)		19 (4.8)
Others	0	44 (0.8)		0
Number of metastatic sites
1	215 (54.4)	2014 (36.9)	<0.0001	214 (54.2)	0.9
2	105 (26.6)	1702 (31.3)		105 (26.6)
≥3	75 (19)	1728 (31.7)		76 (19.3)
Metastatic sites, frequency (%)
Digestive system	196 (32.2)	1859 (21)	<0.0001	193 (31.7)	0.7
Respiratory system	96 (15.8)	1478 (16.7)		102 (16.8)
Bones and joints	68 (11.2)	1207 (13.7)		67 (11)
Brain and other nervous system	24 (3.9)	509 (5.8)		25 (4.1)
Soft tissue (including heart)	19 (3.1)	128 (1.4)		18 (3)
Skin	11 (1.8)	59 (0.7)		9 (1.5)
Lymph nodes	142 (23.3)	2887 (32.7)		143 (23.5)
Ill defined	25 (4.1)	349 (3.9)		26 (4.3)
Others, including buccal cavity and pharynx, breast, female genital system, male genital system, urinary system, hematopoietic and reticuloendothelial systems, endocrine system, and eye and adnexa	28 (4.6)	356 (4)		25 (4.1)
With second primary tumour	18 (4.6)	266 (4.9)	0.7	18 (4.6)	1
Charlson co-morbidity scored	0.3 ± 0.7 (0–6)	0.29 ± 0.72 (0–12)	0.8	0.3 ± 0.6 (0–6)	0.9
>0	92 (23.3)	1194 (21.9)	0.5	93 (23.5)	0.9
0	303	4250		305
1	75	941		77
≥2	17	253		16

Data are presented as mean ± standard deviation (range) or number of patients (%) unless otherwise indicated

CKP cancer from a known primary tumour, CUP cancer of unknown primary tumour, NHLs non-Hodgkin’s lymphomas

aPatients with CUP (n = 395) vs. all CKP (n = 5444) using Fisher’s exact or Chi squared tests. All statistical tests were two sided, and results were considered significant at the 5% critical level. Statistical analysis was performed using SAS, version 9.3 (Cary, NC, USA)

bPatients were matched on the estimated propensity score

cPatients with CUP (n = 395) vs. matched CKP (n = 5444) using Fisher’s exact or Chi squared tests

dCo-morbid diagnoses were considered present if they were found during 1 year before and 6 months after the initial diagnosis with cancer

The diagnostic tests and procedures undertaken during the diagnostic workup for the CUP group compared with the CKP matched group and all patients with CKP in our cohort are described in Table S1 in the ESM. During the diagnostic workup, compared with the matched CKP group, the CUP group were more likely to receive colonoscopy, gastroscopy and/or esophagogastroduodenoscopy, laryngoscopy and pharyngoscopy, laparotomy, panendoscopy (respiratory system); CT scans of the neck, abdomen and pelvis, and spine; MRI scans of the spine; ultrasound scans of the chest, abdomen and retro-peritoneum, female pelvis, miscellaneous scans (Doppler studies); thyroid biopsy; and mammography (Table S1). However, CUP patients were less likely to receive bronchoscopy, mediastinoscopy, proctosigmoidoscopy and pulmonary function tests than were the matched CKP group (Table S1). Other diagnostic tests and procedures were similar between the two patient groups (Table S1).

Treatment Characteristics

Compared with matched CKP patients, patients with CUP were less likely to have surgical resections (mean difference 18.5%; 95% CI 11.8–25; p < 0.0001), receive radiotherapy (mean difference 9.1%; 95% CI 2.5–15.7; p = 0.007) and receive systemic therapy (mean difference 9.1%; 95% CI 2.2–16; p = 0.009) (Table 4). Time to any of these therapies after initial diagnosis did not differ significantly between the CUP and matched CKP groups (Table 4). Among all patients who received systemic therapy, CUP patients were less likely than matched patients with CKP to receive hormone therapy (mean difference 4.5%; 95% CI 1.9–7.1; p = 0.002) and biological targeted therapy (mean difference 13.9%; 95% CI 5.3–22.4; p = 0.002) but more likely to receive platinum drugs (mean difference 11.2%; 95% CI 1.4–20.9; p = 0.02) and taxanes (mean difference 18%; 95% CI 8.2–27.7; p = 0.0003) (Table 4). Table 4 shows the treatment characteristics of the CUP group, matched CKP group and all patients with CKP.

Table 4

Treatments of 5839 patients diagnosed with metastatic cancer by diagnostic status of their primary tumours

Characteristic	Patients with CUP (n = 395)	Patients with CKP (n = 5444)	p valuea	Matched patients with CKP (n = 395)b	p valuec
With surgical resection	112 (28.3)	2673 (49.1)	<0.0001	185 (46.8)	<0.0001
Months between initial cancer diagnosis and surgical resection
Mean ± SD (range)	1.5 ± 3 (0–20.5)	1.7 ± 3.1 (0–24)	0.6	1.2 ± 1.9 (0–15.8)	0.3
≥ 0 to < 3	91	2222		162
≥ 3 to < 6	13	256		17
≥ 6 to < 12	6	134		5
≥ 12 to < 24	2	61		1
With radiotherapy	117 (29.6)	1968 (36.1)	0.009	153 (38.7)	0.006
Months between initial cancer diagnosis and start of radiotherapy
Mean ± SD (range)	4.1 ± 4.7 (0–23.7)	5.2 ± 5.4 (0–24)	0.01	4.6 ± 4.7 (0–22.9)	0.34
≥ 0 to < 3	72	955		78
≥ 3 to < 6	17	402		30
≥ 6 to < 12	20	379		32
≥ 12 to < 24	8	232		13
Type of radiotherapy
Teletherapy	117 (100)	1775 (90.2)	0.001	132 (86.3)	<0.0001
Brachytherapy	0	18 (0.9)		4 (2.6)
Teletherapy + brachytherapy	0	40 (2)		3 (2)
Other types	0	14 (6.9)		14 (9.1)
With systemic therapy	207 (52.4)	3528 (64.8)	<0.0001	243 (61.5)	0.009
Type of systemic therapy received
Only CTX with or without biological targeted therapy	207 (100)	3298 (93.5)	0.0001	232 (95.5)	0.002
HTd + CTX with or without biological targeted therapy	0	230 (6.5)	0.0001	11 (4.5)	0.002
Months between initial cancer diagnosis and start of radiotherapy
Mean ± SD (range)	3 ± 3.6 (0–22.9)	3.4 ± 3.8 (0–23.8)	0.1	3 ± 3.2 (0–18.3)	0.8
≥ 0 to < 3	146	2261		162
≥ 3 to < 6	36	791		58
≥ 6 to < 12	16	295		11
≥ 12 to < 24	9	181		12
With information about CTX and biologic therapy agents received	151 (72.9)	2613 (74)	0.2	180 (74)	0.1
With biological targeted therapy	21 (13.9)	522 (20)	0.06	50 (27.8)	0.002
Type of CTX agents received
Platinum drugse	115 (76.2)	1528 (58.5)	<0.0001	117 (65)	0.02
Alkylating agents	3 (2)	44 (1.7)		1 (0.6)	0.3
Antimetabolitesf	78 (51.7)	1316 (50.4)	0.7	88 (48.9)	0.6
Anthracyclinesg	21 (13.9)	420 (16.1)	0.4	20 (11.1)	0.4
Topoisomerase inhibitorsh	41 (27.2)	793 (30.3)	0.4	60 (33.3)	0.2
Taxanesi	59 (39.1)	467 (17.9)	<0.0001	38 (21.1)	0.0003
Vinca alkaloids	1 (0.7)	175 (6.7)	0.003	7 (3.9)	0.06
Corticosteroids	4 (2.6)	16 (0.6)	0.004	1 (0.6)	0.2
Other anti-tumour antibioticsj	3 (2)	72 (2.8)	0.6	1 (0.6)	0.3
Type of biological targeted therapy agents received
Bevacizumab	4 (2.6)	153 (5.9)	0.09	20 (11.1)	0.003
Rituximab	12 (7.9)	295 (11.3)	0.2	22 (12.2)	0.2
Cetuximab	2 (1.3)	26 (1)	0.6	4 (2.2)	0.5
Interferon-alfa-2b	2 (1.3)	14 (0.5)	0.2	2 (1.2)	0.6
Panitumumab	1 (0.6)	18 (0.7)	0.9	0	0.4
Bortezomib	0	7 (0.3)	0.9	0
Other targeted therapy	1 (0.6)	21 (0.8)	0.9	4 (2.2)	0.3
With support drugs to control CTX-associated side effects or conditions	99 (65.6)	1580 (60.5)	0.2	114 (63.3)	0.7

Data are presented as mean ± SD (range) or number of patients (%) unless otherwise indicated

CKP cancer from a known primary tumour, CTX chemotherapy, CUP cancer of unknown primary tumour, SD standard deviation

aPatients with unknown primary (n = 395) vs. all known primary (n = 5444) using Fisher’s exact or Chi square. All statistical tests were two sided and results were considered significant at the 5% critical level. Statistical analysis was performed using SAS, version 9.3 (Cary, NC)

bPatients were matched on the estimated propensity score

cPatients with unknown primary (n = 395) vs. matched known primary (n = 5444) using Fisher’s exact or Chi square

dHormone therapy included abiraterone, buserelin, leuprolide, letrozole, zoladex, and bicalutamide

ePlatinum drugs included carboplatin, cisplatin and oxaliplatin

fAntimetabolites included capecitabine, gemcitabine, 5-fluorouracil, and raltitrexed

gAnthracyclines included doxorubicin and epirubicin

hTopoisomerase inhibitors included etoposide and irinotecan

iTaxanes included paclitaxel and docetaxel

jOther agents included dexamethasone, vincristine, streptozocin, cyclophosphamide, and mitomycin

Survival Outcomes

The OS of patients with CUP was worse than that of matched CKP patients (2-year OS 41.7 vs. 50.4%, p = 0.005, Fig. 1; HR 1.31, 95% CI 1.1–1.58, p = 0.005, Table 5). In a Cox proportional hazard regression analysis, having a CUP compared with CKP became a non-significant independent predictor of OS when controlling for use of surgery, radiotherapy and systematic therapy (Table 5). In this analysis, receipt of surgical resection and systemic therapy were significant independent predictors of OS (Table 5). No interactions between treatments and primary tumour status (CUP vs. CKP) were identified.

Fig. 1

Overall survival analyses comparing patients with cancer of unknown primary tumour (CUP) with patients with cancer from a known primary tumour (CKP)

Table 5

Adjusted and unadjusted hazard ratios and 95% confidence intervals for death

Proportional hazard modelsa	Unadjusted for tx characteristics		Adjusted for receipt of surgical resection, radiotherapy, and systemic therapy
	CUP vs. CKP	p value	CUP vs. CKP	p value	Surgical resection: no vs. yesb	p value	RTX: no vs. yesb	p value	Systemic therapy: no vs. yesb	p value
For pts with CUP and matched pts with CKP (1:1 matching; n = 790)	1.31 (1.1–1.58)	0.005	1.12 (0.92–1.35)	0.26	2.46 (1.97–3.08)	<0.0001	0.98 (0.84–1.15)	0.2	1.41 (1.16–1.71)	0.0004
For pts with CUP and all pts with CKP (n = 5839)
Unadjusted for pt and disease characteristics	1.29 (1.13–1.47)	0.0002	1.1 (0.96–1.26)	0.18	2.12 (1.96–2.29)	<0.0001	0.95 (0.92–1.02)	0.1	1.39 (1.29–1.5)	<0.0001
Adjusted for pt and disease characteristicsc	1.14 (0.99–1.3)	0.06	1.03 (0.9–1.16)	0.7	2.12 (1.94–2.3)	<0.0001	0.93 (0.89–1.01)	0.1	1.28 (1.18–1.39)	<0.0001
Adjusted for the estimated propensity score	1.16 (1.006–1.32)	0.004	1.02 (0.9–1.18)	0.73	2.1 (1.94–2.26)	<0.0001	0.95 (0.91–1.02)	0.1	1.36 (1.26–1.46)	<0.0001
Adjusted for pt and disease characteristics using inverse probability weighting by the inverse of the propensity score	1.35 (1.22–1.51)	<0.0001	1.18 (1.06–132)	0.002	2.12 (1.95–2.3)	<0.0001	0.94 (0.88–1.00)	0.1	1.3 (1.2–1.41)	<0.0001

Data are presented as hazard ratio (95% confidence interval) unless otherwise indicated

CKP cancer from a known primary tumour, CUP cancer of unknown primary tumour, pt(s) patient(s), RTX radiotherapy, tx treatment

aWe created time-dependent covariates by creating interactions of the covariates and a function of survival time in the models to test proportionality. When time-dependent covariates were not significant, covariates were considered proportional. The proportionality assumption was appropriate for all

bWe tested the interaction between receipt of a given treatment (no vs. yes) and status of primary tumour (CUP vs. CKP) for significance and found none

cPt and disease characteristics included age, sex, co-morbidity, number and type of metastatic sites, grade differentiation, histology, and year of initial diagnosis

In subgroup analysis that included only patients treated with systematic therapy from the CUP and matched CKP groups and controlled for use of surgery and radiotherapy, receipt of a biological targeted therapy was associated with survival advantage (HR 0.52; 95% CI 0.31–0.88; p = 0.01). The type of chemotherapeutic agents received (platinum with or without taxanes vs. other chemotherapeutic combinations) and receipt of hormone therapy were not independent significant predictors of OS. No interactions between these therapies and primary tumour status (CUP vs. CKP) were identified.

Unadjusted and adjusted Cox proportional hazard regression analyses that compared the OS of the CUP group (n = 395) with that of all patients with CKP (n = 5444) revealed similar results (Fig. 1; Table 5).

Direct Costs of Healthcare Utilization

The estimated mean net total costs for the CUP group and matched CKP group were $CAN38,900 and $CAD38,850, respectively. The mean net costs in the “initial diagnostic workup before diagnosis” phase, “continuing diagnostic workup after diagnosis and initial cancer care” phase, “continuing cancer care” phase, and “last 6 months of life” phase accounted for 20.2, 46.5, 14.8 and 18.5% of the total mean net cost for the CUP group, respectively, and for 8.7, 49.5, 26 and 16% of the total mean net cost for the matched CKP group, respectively. Figure 2 depicts the mean cost per day within each phase of care and the mean net cost of an entire phase of care by cost category for the CUP group, matched CKP group and all patients with CKP in the full cohort.

Fig. 2

Cost of healthcare utilization for 5839 patients diagnosed with metastatic cancer by diagnostic status of their primary tumour and cost category and phase of care. Mean net cost of an entire phase of care = (mean cost per day in that phase of care − mean cost per day in the “usual care before the onset of signs of illness” phase) × average number of days spent in that phase of care. Since all patients included in our study survived at least 6 months following their initial cancer diagnosis, the three patient groups spent 2.5 years in the “usual care before the onset of signs of illness” phase and 6 months in the “initial diagnostic workup before diagnosis” phase. In the “continuing diagnostic workup after diagnosis and initial cancer care” phase, CUP patients, matched CKP patients and all patients with CKP spent an average of 144 days, 154 and 156 days, respectively. In the “continuing cancer care” phase, CUP patients, matched CKP patients and all patients with CKP spent an average of 260, 310 and 301 days, respectively. In the “last 6 months of life” phase, CUP patients, matched CKP patients and all patients with CKP spent an average of 108, 95 and 97 days, respectively. Asterisk We used the resource intensity weights [36, 37] recorded for inpatient stays and day procedure group weights [36, 37] recorded for day procedure stays to reflect the resources consumed during hospital contacts. We converted these weights into Canadian dollars using a multiplier known as the cost per weighted case [36, 37]. CKP cancer from a known primary tumour, CUP cancer of unknown primary tumour

Within the “initial diagnostic workup before diagnosis” phase, compared with matched CKP patients, CUP patients had a significant increase in the mean net cost of inpatient and 1-day procedure stays (mean difference $CAD2960; 95% CI 650–5270), a significant increase in the mean net cost of physician and other healthcare provider services (mean difference $CAD1425; 95% CI 1008–1840), and a significant increase in the mean net cost of prescription drugs (mean difference $CAD241; 95% CI 75–406), accounting for a significant increase in the mean net cost of overall healthcare utilization within this phase of care (mean difference $CAD4622; 95% CI 1730–7520) (Fig. 2).

Within the “continuing diagnostic workup after diagnosis and initial cancer care” phase, compared with matched CKP patients, CUP patients had a non-significant difference in the mean net cost of inpatient and 1-day procedure stays and physician and other healthcare provider services but had a significant decrease in the mean net cost of intravenous oncology drugs (mean difference $CAD870; 95% CI 255–1480) and a significant decrease in the mean net cost of prescription drugs (mean difference $CAD340; 95% CI 84–595), accounting for a non-significant difference in the mean net cost of overall healthcare utilization within this phase of care (Fig. 2).

Within the “continuing cancer care” phase, compared with matched CKP patients, CUP patients had a non-significant difference in the mean net cost of inpatient and 1-day procedure stays, a significant decrease in the mean net cost of physician and other healthcare provider services (mean difference $CAD580; 95% CI 290–875), a significant decrease in the mean net cost of prescription drugs (mean difference $CAD450; 95% CI 135–760), and a significant decrease in the mean net cost of intravenous oncology drugs (mean difference $CAD1912; 95% CI 1090–2740), accounting for a significant decrease in the mean net cost of overall healthcare utilization within this phase of care (mean difference $CAD4390; 95% CI 1100–7680) (Fig. 2).

Within the “last 6 months of life” phase, compared with matched CKP patients, CUP patients had a non-significant difference in the mean net cost of inpatient and 1-day procedure stays, physician and other healthcare provider services and intravenous oncology drugs and a significant increase in the mean net cost of prescription drugs (mean difference $CAD477; 95% CI 320–610), accounting for a non-significant difference in the mean net cost of overall healthcare utilization within this phase of care (Fig. 2).

Cost analyses that compared the CUP group with all patients with CKP (n = 5444) across all cost categories and phases of care revealed similar results (Fig. 2).

Discussion

Through a population-based analysis, we found CUP to be the fifth most common (6.8%) cancer type diagnosed in patients presenting with metastatic cancer and to be more common in women (8.8%) than in men (5.3%). The most common histological subtypes found in CUP were adenocarcinoma (40%), undifferentiated carcinoma (29%) and squamous carcinoma (12%). Although CUP patients appeared to undergo more diagnostic tests and procedures during the diagnostic workup than their matched CKP counterparts, patients with CUP did not have their LP tumour site identified, except in 42% of patients where it was discovered at a later phase of care (i.e. after 6 months from initial cancer diagnosis). The percentage of LP tumour detection later in the course of the disease in our CUP group was higher than previously reported estimates [9], which was likely due to our conservative inclusion criteria of at least 6-month survival.

Having CUP appears to be associated with less frequent use of surgical interventions, radiation and hormonal and biological targeted therapy as well as greater use of non-selective cytotoxic chemotherapeutic drugs such as platinum drugs and taxanes. There was a significant decrease in the mean net cost of overall healthcare utilization, including the cost of intravenous oncology drugs during the “continuing cancer care” phase. Less exposure to surgery and biological targeted therapy were independently associated with higher risk of death and appeared to account for most of the observed 31% increase in risk of mortality for patients with CUP. This association should be interpreted with caution as it might also be influenced by unknown differences in tumour biologic behaviour, disease burden and/or the functional status of patients between the CUP and matched CKP groups [45]. However, no evidence exists yet showing CUP tumours harbour distinct genetic traits compared with CKP tumours [6, 46]. Thus, it might be reasonable to infer that many patients were considered unsuitable for more specific targeted cancer treatments and were treated with more intensive empiric cytotoxic chemotherapy due to the absence of knowledge about their primary tumour site. Therefore, these data suggest that identification of the primary tumour site early in the course of metastatic disease may enable greater precision of cancer therapy and potentially improve patients’ survival by allowing patients with CUP to benefit more from available healthcare resources during the “continuing cancer care” phase, similar to their counterparts with CKP [29].

Currently, a precision medicine approach can be applied to the treatment of many metastatic cancers, including cetuximab and panitumumab in colorectal cancer [27], rituximab in lymphoma [47], bevacizumab in renal cell carcinoma [48] and colorectal cancer [49], trastuzumab in breast cancer [50], erlotinib in lung cancer [51] and sorafenib and sunitinib in renal cell carcinoma [52]. Knowledge of the biologic characteristics of an individual tumour (e.g. somatic EGFR, KRAS, ALK, HER2, BRAF, CD20, and ROS1 gene status) is increasingly valuable in the clinical management and treatment selection for patients with metastatic cancer [27, 47–52]. However, the ability to identify a primary tumour site is also increasingly important and likely to remain important for the foreseeable future [8]. For instance, knowledge of the primary tumour site is needed to interpret somatic mutation results. Information about KRAS mutation status has quite different implications depending on whether the primary site is lung versus colon [53]. Similarly, information regarding hormone receptor status has quite different implications depending on whether the primary tumour site is breast or ovary. Generally, targeted therapies are studied, approved and reimbursed solely within the context of an identified primary tumour site [27, 47–52]. Furthermore, finding the primary tumour site might prevent local complications (e.g. bleeding from the primary tumour, obstruction or perforation of a viscus), give a better guide to prognosis and help integrate patient-centred care into practice by helping the physician communicate with the patient, who may also find value in knowing where their cancer originated from, independent of effects on prognosis and treatment [6, 46]. Therefore, information about the primary tumour site and its inherent biologic characteristics are both valuable and complementary in precision management of patients with CUP [6, 46].

In our study, having CUP was associated with a significant increase in the mean net cost of overall healthcare utilization during the “initial diagnostic workup before diagnosis” phase. Patients with CUP were also more likely than those with CKP to receive several diagnostic tests and procedures during the diagnostic workup. These findings indicate that patients with CUP underwent more extensive diagnostic investigations and incurred more costs to the healthcare system related to difficulties in diagnosis. Despite this, they remained without a primary tumour classification following their clinical and pathologic diagnostic workup, according to our study of real-life Canadian clinical practice. Although data about IHC investigation were not available and thus our study was unable to investigate pathological diagnostic barriers in these patients, current Canadian clinical practice has not been influenced by the availability of accurate gene expression profiling assays to help identify the primary tumour in metastatic cancer [1, 10, 54]. Our data suggest the need for gene expression profiling techniques to complement current traditional diagnostic procedures (e.g. IHC analyses, endoscopies, CT scans, X-rays, MRI scans, etc.) when dealing with diagnostic difficulties so that the primary tumour can be classified early in the course of metastatic disease. This may allow patients to avoid unnecessary or even painful and distressing extensive investigations and the healthcare system to avoid unnecessary costs. Recently, the use of a gene expression profiling test to aid in identifying the primary tumour when current clinical and pathological diagnostic evaluation failed to provide a diagnosis of primary tumour site in CUP patients was found to be cost effective from the Canadian healthcare system perspective [34]. Our data further suggest some value may be gained from using gene expression profiling techniques at earlier stages in the diagnostic workup.

Although this is a retrospective cohort study and our results must be interpreted with caution, the incidence of CUP and the impact of primary tumour classification on therapy, patient outcomes and cost of care throughout the course of metastatic disease are unlikely to be studied in prospective designed analyses or randomized controlled trials. This is because CUP syndrome is extremely heterogeneous and the ultimate study design would require a very large sample size. Randomization to either site-specific therapy or standard CUP empiric therapy following primary tumour classification also may not be ethical because it is already believed that, for many primary tumour diagnoses, the standard empiric therapy for CUP would be less effective. Our retrospective cohort study is an example of an alternative approach.

This study used rigorous linkage of high-quality population data from comprehensive heath administrative databases and yielded a true incidence rate of CUP given our strict inclusion criteria of histologically confirmed metastatic disease and at least 6-month survival. We took special care to avoid sources of bias and confounding in our study by conducting a matched cohort analysis where the matched group of patients with CKP clearly had the same underlying population of Manitoba as patients with CUP and were matched on all known patient and tumour characteristics. In fact, the smaller number of patients included in our matched cohort analysis compared with our overall cohort permits future investigation of more detailed and risk factors of having a CUP. For instance, important factors associated with diagnostic workup obtained from detailed medical histories or biologic markers such as specialist referrals and type and frequency of immunohistochemistry tests (i.e. information not collected by the databases used for this study) become feasible to investigate in order to understand the actual diagnostic barriers in patients with CUP. Future studies can further link such real-life cases with their specimens from banks of tumour tissue samples to study the potential utility of personalized diagnostic technologies such as the newly developed gene expression profiling assays.

In addition, the diagnostic and prognostic parameters and phase-specific cost estimates described in our study represent key imputes necessary to build decision analytic models designed to evaluate the cost effectiveness of such personalized diagnostic technologies in CUP. Developing these data is important to formulate new provincial guidelines and reimbursement policies for CUP management and is necessary to inform healthcare resource allocation and fiscal planning for the prospective precision medicine era of care for CUP. Thus, our data will ultimately contribute in developing additional clinical evidence to optimize a precision medicine strategy as a standard of care for patients with CUP.

Conclusion

CUP is the fifth most common cancer type diagnosed in patients presenting with metastatic cancer and is more common in women than in men. Compared with CKP patients, CUP patients receive fewer site-specific and targeted therapies but more empiric therapies, have reduced OS, and use more healthcare resources for diagnostic workup but less healthcare resources for cancer care. Identifying the primary tumour in CUP patients might enable the use of more precise anticancer therapy with the goals of improving OS and more efficiently allocating healthcare resources.

Below is the link to the electronic supplementary material.

Supplementary material 1 (DOC 24 kb)

Supplementary material 2 (DOC 136 kb)

Cancer of unknown primary tumour (CUP) is the fifth most common cancer type in patients presenting with metastatic cancer.

Compared with patients with metastatic cancer of known primary, patients with CUP receive fewer site-specific cancer treatments, have reduced overall survival, and use more healthcare resources for diagnostic workup but less healthcare resources for cancer care.

Identifying the primary tumour in CUP patients might enable the use of more precise anticancer therapy, improve overall survival and allow more efficient allocation of healthcare resources.

The use of accurate genomic tests to help identify the primary tumour in CUP might be clinically and economically warranted.