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. 2022 Jan 10;2022:2066133. doi: 10.1155/2022/2066133

Increased Risk of Suicide among Cancer Survivors Who Developed a Second Malignant Neoplasm

Huazhen Yang 1,2, Yuanyuan Qu 1,2, Yanan Shang 1,2, Chengshi Wang 3,4, Junren Wang 1,2, Donghao Lu 1,5,6,, Huan Song 1,2,7,
PMCID: PMC8763535  PMID: 35047029

Abstract

Background

Cancer diagnosis entails substantial psychological distress and is associated with dramatically increased risks of suicidal behaviors. However, little is known about the suicide risk among cancer survivors who developed a second malignant neoplasm (SMN).

Methods

Using the Surveillance, Epidemiology, and End Results database, we conducted a population-based cohort study involving 7,824,709 patients with first malignant neoplasm (FMN). We measured the hazard ratios (HRs) of suicide death after receiving a SMN diagnosis using Cox proportional hazard models, as compared with patients with FMN. The comparison with the US population was achieved by calculating standardized mortality ratios (SMRs).

Results

Totally 685,727 FMN patients received a diagnosis of SMN during follow-up, and we in total identified 10,930 and 937 suicide deaths among FMN and SMN patients, respectively. The HR of suicide deaths was 1.23 (95% confidence interval (CI), 1.14–1.31) after a SMN diagnosis, compared with FMN patients, after adjusting for sociodemographic factors, tumor characteristics, and cancer treatment. As compared with the general population, while both SMN and FMN patients suffered an increased risk of suicide deaths, the excess risk was higher among SMN patients than FMN patients (age-, sex-, and calendar-year-adjusted SMR 1.65 (95% CI 1.54–1.75) vs. 1.29 (95% CI 1.26–1.31); Pdifference < 0.0001). Notably, across different time periods, we observed the greatest risk elevation during the first 3 months after a cancer diagnosis.

Conclusions

Compared with either patients with FMN or the general population, cancer survivors who received a SMN diagnosis were at increased risk of suicide death. The risk elevation was most prominent soon after the cancer diagnosis, highlighting the necessity of providing timely psychological support to cancer survivors with a SMN.

1. Introduction

A growing number of patients are surviving from cancer because of the increased survival as well as the advances in cancer screening programs and novel treatments [13]. However, all cancer survivors are at risk for developing a second primary cancer [46]. It was reported that the incidence of second malignant neoplasm (SMN), calculated from the Surveillance, Epidemiology, and End Results (SEER) Program, was approximately 8.1% between 1992 and 2008 in the United States, indicating that nearly 1 in 12 cancer patients can develop a SMN [6].

Cancer is a devastating illness that comes with tremendous psychological distress [79]. Accumulating evidence has shown that people diagnosed with cancer are at an elevated risk of suicidal behaviors, including complete suicide [1012] and suicide attempts [13, 14], compared with the general population. Therefore, it is plausible that receiving a diagnosis of SMN, acting as a repeat and possibly stronger stressor, might further increase the risk of suicide among cancer survivors. Indeed, patients with subsequent primary cancers (i.e., two or more primary cancers) have been reported to be at elevated risk for poorer physical and mental health status (e.g., serious psychological distress) [1518]. However, the risk of suicide among patients with SMN is unclear.

Therefore, leveraging the population-based cancer cohort from the SEER database, which has stringent criteria for identifying multiple primary neoplasms, together with the aggregated US population data and US mortality data, we aimed to examine the risk of suicide among cancer survivors who developed a SMN.

2. Materials and Methods

2.1. Study Population

The SEER Program has collected cancer incidence and survival data from population-based cancer registries since 1973, covering approximately 34% of the US population as of 2016 [19]. Information on patient demographics, year and month of diagnosis, tumor characteristics (including primary tumor site, cancer behavior, tumor size, and tumor grade), treatment utilization, and active follow-up for vital status were routinely documented [20].

In the present study, we conducted a population-based cohort study using the SEER registry records between January 1, 1975, and December 31, 2016, in the United States. Among the 9,157,072 cancer patients (Figure 1), we excluded 114,866 who were diagnosed only through autopsy or death certificate, 1,409 with no information on birth year, 1,184,919 that recorded as not their first malignancy (670,225 with no information on primary malignancy and 514,694 with no information on FMN), and 31,169 with their cancer diagnosis before age 5, leaving 7,824,709 eligible FMN patients for further analysis.

Figure 1.

Figure 1

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Study design.

All patients were followed from the diagnosis of FMN until death, the occurrence of a subsequent malignancy, or December 31, 2016, whichever occurred first. Because the SEER data provided only survival in months for survival analysis, we assigned an average survival time of 15 days for individuals who died in the same month of diagnosis. By linking to the subsequent malignancy diagnoses in SEER, we identified 685,727 patients who developed a SMN during the follow-up who therefore were included in the exposed group. Namely, patients without a SMN diagnosis contributed all person-time to the unexposed group, while the ones with a SMN diagnosis contributed their person-time before the SMN diagnosis to the unexposed group and to the exposed group from the time of diagnosis onward.

2.2. Ascertainment of FMN and SMN

We first identified patients with a FMN diagnosis according to the SEER collected tumor information on the primary tumor (yes or no), tumor behavior (malignant or not), and first malignant primary indicator (yes or no). Through linkage to the information on subsequent cancer diagnoses, we then further identified individuals with a SMN diagnosis among these FMN survivors. In a subanalysis, we performed separate analyses on prostate cancer, breast cancer, colorectal cancer, lung cancer, nonmelanoma skin cancer, cancer of the central nervous system, severe cancer (esophageal, liver, or pancreatic cancer), and other cancers, as well as lifestyle-related cancers (alcohol- and smoking-related cancers) [21], according to the International Classification of Disease Oncology (ICD-O) third edition codes (Supplementary Table 1).

2.3. Ascertainment of Suicide

Based on the cause-specific death classification both for SEER and US mortality data, which was derived from the death certificate, we considered individuals to have committed suicide if the cause of death was coded as suicide and self-inflicted injury, with the corresponding International Classification of Diseases (ICD) 10th edition (ICD-10) codes as U03, X60-X84, and Y87.0.

2.4. Covariates

Data on potential confounders, including birth year, sex, calendar year at diagnosis, sociodemographic factors (i.e., race, cohabitation status, insurance, and state), tumor characteristic (i.e., tumor size and grade), and cancer treatment (i.e., chemotherapy, radiotherapy, and surgery), were obtained from the SEER database. All missing values of the covariates were coded to the “unknown” category. The corresponding information on age at death, sex, and calendar year for the US population data were derived from the US Census Bureau's Population Estimates Program.

2.5. Statistical Analysis

We assessed the relative risk of suicide in relation to SMN diagnosis compared with FMN patients, using hazard ratios (HRs) with 95% confidence intervals (CI) derived from Cox regression models. Models were partly (models 1–3) or fully (model 4) adjusted for the birth year (as a continuous variable), sex (male or female), calendar year at diagnosis (1975–1984, 1985–1994, 1995–2004, or 2005–2016), race (white, black, or others/unknown), cohabitation status (cohabitation, noncohabitation, or unknown), insurance (insured, uninsured, or unknown), state (Alaska, California, Connecticut, Georgia, Hawaii, Iowa, Kentucky, Louisiana, Michigan, New Jersey, New Mexico, Utah, or Washington), tumor size (<1.5, ≥1.5 cm, or unknown), tumor grade (well, moderately, poorly differentiated/undifferentiated, or unknown), chemotherapy/radiotherapy (yes or no/unknown), and surgery (yes or no/unknown). We also examined the association between SMN diagnosis and subsequent risk of suicide death by cancer subtypes, after controlling for available confounders. Lifestyle factors (i.e., alcohol drinking and smoking) might modify the studied association. We therefore also separately analyzed alcohol-related cancers and smoking-related cancers.

In subgroup analyses, HRs were calculated separately by age at diagnosis (by quantile: <55, 55–65, 66–75, or >75 years), calendar year at diagnosis, sex, race, cohabitation status, tumor size, tumor grade, chemotherapy/radiotherapy, surgery, and the time interval between FMN and SMN. Furthermore, we explored whether the relative risk of suicide after a SMN diagnosis varied across different time periods since cancer diagnosis, by analyzing the associations in different follow-up periods (<1, 1–2, 3–4, 5–10, or >10 years). Additionally, we calculated the HRs by characteristics of their first malignancies (i.e., tumor characteristics and treatment utilization) to explore the potential modified role of first malignancy among SMN patients. The statistical significance of the difference between HRs was assessed by including an interaction term in the Cox model.

To better interpret our findings, we also calculated standardized mortality ratios (SMRs; i.e., the ratio of the observed to the expected number of suicide deaths) with 95% CIs to estimate the relative risk for suicide after SMN, as well as FMN, using the general US population as reference. Specifically, the number of expected suicide deaths was calculated by multiplying the observed number of person-years by age- (5 year strata), sex-, and calendar-year-specific suicide rates derived from the general US population. We further estimated SMRs by different follow-up periods (i.e., ≤1, 2–3, 4–6, or 7–12 months or 1–2, 3–5, 6–10, or >10 years) after the SMN or FMN diagnosis to examine the immediate and long-term impact. The statistical significance of the difference between SMRs was assessed by the heterogeneity test.

To test the robustness of the observed associations, we repeated the main analysis excluding SMN patients with a prior history of FMN at the same tumor site. We further assessed the potential influence of unmeasured confounders using the E-value [22]. All the analyses were conducted in R software (version 4.0). A two-sided P-value <0.05 was considered statistically significant.

3. Results

Of the 9,157,072 cancer patients in the SEER data, we identified 7,824,709 FMN patients in the population-based cohort, among which 685,727 individuals were exposed to a SMN diagnosis during up to 42 years of the follow-up period (Figure 1). With a total of 46,507,112 accumulated person-years, the median follow-up time was 1.67 (Q1–Q3: 0.42–5.00) and 3.17 (0.67–8.67) years for the SMN and FMN patients, respectively (Table 1). There was little difference in race, cohabitation status, state, and tumor grade between the SMN and FMN patients. However, compared with the FMN patients, patients with a SMN diagnosis were more likely to be male (58.97% vs. 51.28%), older (mean age 71.00 vs. 63.60 years), insured (49.46% vs. 38.82%), with larger tumor size (46.92% vs. 42.31%), and not treated (37.35% vs. 44.32% and 53.46% vs. 58.59% for chemotherapy/radiotherapy and surgery, respectively).

Table 1.

Characteristics of the study cohort.

SMNa(N = 685727) FMNb(N = 7824709)
Follow-up time, mean (SD), y 3.50 (4.47) 5.64 (6.53)
Follow-up time, median (Q1–Q3), y 1.67 (0.42–5.00) 3.17 (0.67–8.67)
Birth year, mean (SD), y 1,930 (14.70) 1,940 (18.50)
Age at diagnosis, mean (SD), y 71.00 (11.60) 63.60 (15.10)
Age group (by quantile), no. (%), y
 <55 58,180 (8.48) 1,939,983 (24.79)
 55–66 159,108 (23.20) 2,300,439 (29.40)
 67–75 206,746 (30.15) 1,827,392 (23.35)
 >75 261,693 (38.16) 1,756,895 (22.45)
Calendar year, no. (%)
 1975–1984 26,808 (3.91) 668,993 (8.55)
 1985–1994 74,360 (10.84) 988,075 (12.63)
 1995–2004 163,161 (23.79) 2,194,895 (28.05)
 2005–2016 421,398 (61.45) 3,972,746 (50.77)
Sex, no. (%)
 Male 404,391 (58.97) 4,012,867 (51.28)
 Female 281,336 (41.03) 3,811,842 (48.72)
Race, no. (%)
 White 586,494 (85.53) 6,427,454 (82.14)
 Black 63,114 (9.20) 797,649 (10.19)
 Others/unknown 36,119 (5.27) 599,606 (7.66)
Cohabitation status, no. (%)
 Cohabitation 249,999 (36.46) 2,940,863 (37.58)
 Noncohabitation 390,221 (56.91) 4,351,566 (55.61)
 Unknown 45,507 (6.64) 532,280 (6.80)
Insurance, no. (%)
 Insured 339,146 (49.46) 3,037,767 (38.82)
 Uninsured 3,822 (0.56) 90,885 (1.16)
 Unknown 342,759 (49.98) 4,696,057 (60.02)
State, no. (%)
 Alaska 533 (0.08) 7,495 (0.10)
 California 216,848 (31.62) 2,767,483 (35.37)
 Connecticut 63,227 (9.22) 603,280 (7.71)
 Georgia 56,227 (8.20) 733,285 (9.37)
 Hawaii 15,738 (2.30) 169,385 (2.16)
 Iowa 55,057 (8.03) 508,535 (6.50)
 Kentucky 26,320 (3.84) 337,028 (4.31)
 Louisiana 23,977 (3.50) 320,179 (4.09)
 Michigan 73,514 (10.72) 676,773 (8.65)
 New Jersey 52,786 (7.70) 664,090 (8.49)
 New Mexico 17,921 (2.61) 223,539 (2.86)
 Utah 19,001 (2.77) 220,849 (2.82)
 Washington 64,578 (9.42) 592,788 (7.58)
Cancer sites, no. (%)
 Prostate cancer 70,992 (10.35) 1,186,195 (15.16)
 Breast cancer 45,939 (6.70) 1,188,792 (15.19)
 Colorectal cancer 82,991 (12.10) 835,070 (10.67)
 Lung cancer 121,001 (17.65) 975,192 (12.46)
 Skin (nonmelanoma) 4,064 (0.59) 28,036 (0.36)
 CNSc cancer 6,630 (0.97) 113,471 (1.45)
 Severe cancerd 40,647 (5.93) 388,774 (4.97)
 Other cancers 258,521 (37.70) 2,526,393 (32.29)
Smoking-related cancers
 No 434,306 (63.34) 5,814,303 (74.31)
 Yes 251,421 (36.66) 2,010,406 (25.69)
Alcohol-related cancers
 No 648,254 (94.54) 7,467,584 (95.44)
 Yes 37,473 (5.46) 357,125 (4.56)
Tumor size, no. (%), cm
 <1.5 66,741 (9.73) 791,353 (10.11)
 ≥1.5 321,740 (46.92) 3,310,859 (42.31)
 Unknown 297,246 (43.35) 3,722,497 (47.57)
Tumor grade, no. (%)
 Well differentiated 61,799 (9.01) 734,335 (9.38)
 Moderately differentiated 170,021 (24.79) 2,069,948 (26.45)
 Poorly differentiated/undifferentiated 155,702 (22.71) 1,900,555 (24.29)
 Unknown 298,205 (43.49) 3,119,871 (39.87)
Chemotherapy/radiotherapy
 No/unknown 429,626 (62.65) 4,356,691 (55.68)
 Yes 256,101 (37.35) 3,468,018 (44.32)
Surgery
 No/unknown 319,150 (46.54) 3,240,379 (41.41)
 Yes 366,577 (53.46) 4,584,330 (58.59)
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aSecond malignant neoplasm. bFirst malignant neoplasm. cCentral nervous system. dEsophageal, liver, or pancreatic cancer.

During follow-up, a total of 937 suicide deaths (crude incidence rate, 3.90 per 10,000 person-years) and 10,930 suicide deaths (2.48 per 10,000 person-years) were identified among SMN patients and FMN patients, respectively (Table 2). Correspondingly, we observed a consistently elevated relative risk of suicide among SMN patients compared with FMN patients across different models; the fully adjusted HR (model 4) was 1.23 (95% CI 1.14–1.31). Similar risk elevations were observed for alcohol-related cancers (HR 1.37; 95% CI 1.10–1.72; Figure 2) and smoking-related cancers (HR 1.18; 95% CI 1.06–1.31). Furthermore, among all studied cancer subtypes defined by the sites of SMN, the HRs were most pronounced when SMN was severe cancer (HR 1.97; 95% CI 1.48–2.63) or lung cancer (HR 1.57; 95% CI 1.34–1.86; Figure 2).

Table 2.

Risk of suicide among individuals with a second malignant neoplasm (SMN) diagnosis, by different adjustment strategies, compared with individuals with a first malignant neoplasm (FMN) diagnosis.

Model information No. of suicide cases/no. of accumulated person-years × 10,000 (incidence rate/10,000 person-years) Hazard ratio (95% confidence interval)
SMN FMN
Different adjustment strategiesa
Model 1: adjusted for birth year, sex, and calendar year 937/2,401,152.92 (3.90) 10930/44,105,958.92 (2.48) 1.24 (1.16–1.32)
Model 2: model 1 + sociodemographic factors (i.e., race, cohabitation status, insurance, and state) 1.23 (1.15–1.32)
Model 3: model 2 + tumor characteristics (i.e., tumor size and tumor grade) 1.22 (1.14–1.31)
Model 4 (full model): model 3 + cancer treatment (i.e., chemotherapy/radiotherapy and surgery) 1.23 (1.14–1.31)
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aCox model was used to estimate hazard ratios (HRs), adjusted for covariates listed in the model information column.

Figure 2.

Figure 2

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Risk of suicide among individuals with a second malignant neoplasm (SMN) diagnosis, by cites of SMN or lifestyle-related cancers, compared with individuals with a first malignant neoplasm (FMN) diagnosis. aCox model was used to estimate hazard ratios (HRs), adjusted for birth year, sex, calendar year, race, cohabitation status, insurance, state, tumor size, grade, chemotherapy/radiotherapy, and surgery. bCentral nervous system. cEsophageal, liver, or pancreatic cancer.

In a subanalysis, the excess risk of suicide in SMN patients did not differ by calendar year, sex, race, cohabitation status, tumor grade, tumor size, chemotherapy/radiotherapy, and the time interval between FMN and SMN (Table 3). Likewise, similar estimates were found across different follow-up periods (Pdifference = 0.95; Table 3). However, the HRs were somewhat higher among younger patients (Pdifference = 0.0003) and patients treated with surgery (Pdifference = 0.0011). A greater risk of suicide was also observed in SMN patients who underwent chemotherapy/radiotherapy (Pdifference = 0.013) and surgery (Pdifference = 0.045) for their first malignancy (Table 4).

Table 3.

Risk of suicide among individuals with a second malignant neoplasm (SMN) diagnosis, by different characteristics, compared with individuals with a first malignant neoplasm (FMN) diagnosis.

No. of suicide cases/no. of accumulated person-years × 10,000 (incidence rate/10,000 person-years) Hazard ratioa (95% confidence interval) P difference
SMN FMN
By age at diagnosis (by quantile), y 0.0003
 <55 75/315,337.92 (2.38) 2780/15,810,144.58 (1.76) 1.38 (1.09–1.73)
 55–65 223/687,006.17 (3.25) 3234/13,794,478.21 (2.34) 1.32 (1.15–1.52)
 66–75 339/747,527.17 (4.53) 2816/9,059,181.29 (3.11) 1.33 (1.19–1.50)
 >75 300/651,281.67 (4.61) 2100/5,442,154.83 (3.86) 0.96 (0.85–1.09)
By calendar year, y 0.15
 1975–1984 68/116,017.71 (5.86) 1584/5,375,711.83 (2.95) 1.43 (1.12–1.82)
 1985–1994 191/364,410.29 (5.24) 2296/8,174,559.13 (2.81) 1.40 (1.21–1.63)
 1995–2004 260/789,908.79 (3.29) 3473/16,284,736.13 (2.13) 1.21 (1.06–1.37)
 2005–2016 418/1,130,816.13 (3.70) 3577/14,270,951.83 (2.51) 1.17 (1.05–1.29)
By sex 0.99
 Male 825/1,320,654.54 (6.25) 9030/20,956,633.67 (4.31) 1.20 (1.11–1.29)
 Female 112/1,080,498.38 (1.04) 1900/23,149,325.25 (0.82) 1.20 (0.99–1.46)
By race 0.066
 White 880/2,091,732.79 (4.21) 10060/36,981,749.92 (2.72) 1.23 (1.15–1.32)
 Black 38/181,568.13 (2.09) 368/3,798,398.25 (0.97) 1.70 (1.21–2.41)
By cohabitation status 0.45
 Cohabitation 336/746,244.92 (4.50) 4120/13,911,216.5 (2.96) 1.20 (1.07–1.35)
 Noncohabitation 546/1,493,855.42 (3.65) 5939/27,156,872.79 (2.19) 1.27 (1.16–1.39)
By tumor size, cm 0.057
 <1.5 79/321,027 (2.46) 758/5,869,076.38 (1.29) 1.39 (1.10–1.76)
 ≥1.5 366/1,025,931.79 (3.57) 3640/16,163,041.38 (2.25) 1.08 (0.97–1.21)
By tumor grade 0.81
 Well differentiated 86/306,398.13 (2.81) 1000/5,384,767.58 (1.86) 1.29 (1.03–1.61)
 Moderately differentiated 275/769,611.54 (3.57) 3179/14,044,744.63 (2.26) 1.37 (1.21–1.56)
 Poorly differentiated/undifferentiated 252/473,608.54 (5.32) 2696/8,978,857.25 (3.00) 1.40 (1.23–1.60)
By chemotherapy/radiotherapy 0.91
 No/unknown 630/1,590,770.13 (3.96) 6701/25,942,336.79 (2.58) 1.22 (1.13–1.33)
 Yes 307/810,382.79 (3.79) 4229/18,163,622.13 (2.33) 1.23 (1.09–1.38)
By surgery 0.0011
 No/unknown 397/662,482.42 (5.99) 4654/10,600,572.79 (4.39) 1.07 (0.96–1.18)
 Yes 540/1,738,670.5 (3.11) 6276/33,505,386.13 (1.87) 1.35 (1.23–1.48)
By time interval between FMN and SMN, y 0.84
 ≤1 246/630,900.92 (3.90) 10930/44,105,958.92 (2.48) 1.24 (1.09–1.40)
 2–3 195/464,630.75 (4.20) 10930/44,105,958.92 (2.48) 1.29 (1.12–1.49)
 4–6 189/486,033.92 (3.89) 10930/44,105,958.92 (2.48) 1.19 (1.03–1.38)
 >6 307/819,587.33 (3.75) 10930/44,105,958.92 (2.48) 1.20 (1.07–1.34)
By follow-up periods, y 0.95
 <1 376/509,112.92 (7.39) 3131/6,261,779.63 (5.00) 1.18 (1.06–1.31)
 1–2 153/784,901.33 (1.95) 1510/10,511,420.75 (1.44) 1.26 (1.06–1.49)
 3–4 199/1,328,072.67 (1.50) 2368/20,421,357.75 (1.16) 1.22 (1.06–1.42)
 5–10 143/1,387,784.33 (1.03) 2210/26,923,811.17 (0.82) 1.24 (1.05–1.48)
 >10 66/904,527.5 (0.73) 1711/26,133,082.67 (0.65) 1.28 (1.00–1.63)
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aCox model was used to estimate hazard ratios (HRs), adjusted for birth year, sex, calendar year, race, cohabitation status, insurance, state, tumor size, grade, chemotherapy/radiotherapy, and surgery.

Table 4.

Risk of suicide among individuals with a second malignant neoplasm (SMN) diagnosis, by characteristics of the first malignancy, compared with individuals with a first malignant neoplasm (FMN) diagnosis.

No. of suicide cases/no. of accumulated person-years × 10,000 (incidence rate/10,000 person-years) Hazard ratioa (95% confidence interval) P difference
SMN FMN
By FMN tumor size, cm 0.57
 <1.5 62/260,141.08 (2.38) 758/5,869,076.38 (1.29) 1.55 (0.77–3.12)
 ≥1.5 285/839,718.17 (3.39) 3,640/16,163,041.38 (2.25) 1.26 (1.06–1.50)
By FMN grade 0.54
 Well differentiated 118/318,247.38 (3.71) 1,000/5,384,767.58 (1.86) 1.39 (0.82–2.36)
 Moderately differentiated 334/817,983.33 (4.08) 3,179/14,044,744.63 (2.26) 1.65 (1.37–1.99)
 Poorly differentiated/undifferentiated 212/466,502.54 (4.54) 2,696/8,978,857.25 (3.00) 1.86 (1.47–2.37)
By FMN chemotherapy/radiotherapy 0.013
 No/unknown 590/1,525,397.25 (3.87) 6,701/25,942,336.79 (2.58) 1.28 (1.16–1.41)
 Yes 347/875,755.67 (3.96) 4,229/18,163,622.13 (2.33) 1.64 (1.39–1.95)
By FMN surgery 0.045
 No/unknown 272/512,397.08 (5.31) 4,654/10,600,572.79 (4.39) 1.18 (0.99–1.40)
 Yes 665/1,888,755.83 (3.52) 6,276/33,505,386.13 (1.87) 1.45 (1.31–1.61)
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aCox model was used to estimate hazard ratios (HRs), adjusted for birth year, sex, calendar year, race, cohabitation status, insurance, state, tumor size, grade, chemotherapy/radiotherapy, and surgery.

The calculation of SMRs, using the general US population as a reference, revealed a further increased risk of suicide among SMN patients (SMR 1.65 (95% CI 1.54–1.75)) relative to FMN patients (SMR 1.29 (95% CI 1.26–1.31); Pdifference < 0.0001). Across different follow-up periods, the changing patterns were similar between SMN patients and FMN patients, both of which showed the highest estimates within the first 3 months after cancer diagnosis (Figure 3 and Supplementary Table 2). The excess risk then experienced a rapid decline but remained at a significant level for up to 5 years.

Figure 3.

Figure 3

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Change of the suicide standardized mortality ratios (SMRs) over follow-up periods among patients with first malignant neoplasm (FMN) or second malignant neoplasm (SMN), compared with the general population. The expected number for suicide deaths during the study period was derived from age (5 year groups), sex, and calendar year (1 year groups) suicide death rate for the USA.

In sensitivity analysis, we observed largely comparable results after excluding SMN patients whose first malignancy was at the same tumor site (Supplementary Table 3). In addition, the calculation of the E-value revealed that a minimal magnitude of 1.76-fold increased risk of suicide death that was associated with the unmeasured confounders would be needed to entirely explain the observed association.

4. Discussion

To the best of our knowledge, this is the first large-scale cohort study that examined the risk of suicide among cancer survivors who developed a SMN, using population-based register data in the USA. We found that compared with FMN patients, patients with a SMN diagnosis, particularly those diagnosed at a younger age, with aggressive SMN, or had received surgery treatment for the SMN, were at an increased risk of suicide death within the entire follow-up period after adjusting for many potential confounders. Importantly, as the calculations of relative risk (i.e., SMR) of suicidal death relative to the general US population revealed a high-risk time period (i.e., the first 3 months after SMN diagnosis), such finding highlights the time window for suicide intervention among SMN patients.

The immediate suicide risk following a FMN diagnosis has been well estimated in previous studies, suggesting cancer diagnosis as an acute stressor that can lead to suicide behaviors [11, 13, 23]. Nevertheless, with regard to SMN, data from large longitudinal studies are scarce. We therefore have limited knowledge about the suicide risk among SMN patients, and whether the level of such a risk is comparable or superior to that among FMN patients. In our study, we, for the first time, showed a significant impact of a SMN diagnosis on the subsequent suicide risk, relative to a FMN diagnosis. Despite the absence of comparable data from studies with a similar design, our findings gain support from previous investigations that consistently suggested cancer survivors with multiple primary cancers had more frequent or greater psychological distress than survivors of single cancer, which was measured by the number of days of self-reported mental-health-related feelings in the past month [1517]. Such results indicate that a diagnosis of subsequent primary cancer might bring additional adverse effects on the mental health among cancer survivors. Moreover, in a study also based on the SEER database, it focused on the sex disparity of suicide risk among cancer patients, and the authors reported an increased risk for suicidal death among secondary primary head and neck cancer patients, compared with those with head and neck cancer as the first primary cancer, which is in line with our present results [24]. Furthermore, the comparison with the general population corroborates the findings by illustrating consistently higher SMRs among SMN than FMN patients over time since the diagnosis. Those two groups of patients, however, shared a temporal pattern of suicide death risk, with the period shortly after the cancer diagnosis (i.e., within 3 months for both SMN and FMN) as a high-risk time period with the most frequent suicide deaths. The observed temporal pattern was in accordance with our previous findings on the risk patterns of mental disorders after the cancer diagnosis [8]. These results further indicate the psychological stress induced by the diagnosis of the subsequent malignant neoplasm and call for attention to monitor the mental health status of cancer survivors, especially for those who experienced a recent diagnosis of cancer, and to carry out necessary thought interventions, such as initiating timely psychosocial care [25] and providing prompt suicide risk screening [26].

Besides the repeated exposure to a notorious stressful event such as cancer diagnosis [27], other explanations for the phenomenon that SMN patients might suffer from a higher level of psychological stress, in comparison with FMN patients, include poorer mental health status (e.g., being more likely to have the serious psychological disorder) [15], worse overall health condition (e.g., being reported more health-related bed days) [15], poorer quality of life [28], and undermined socioeconomic status due to the treatment of FMN [29]. In addition, even if patients eventually survived their cancer, cancer treatment itself could be invasive and painful and often accompanied by severe side effects that could traumatize cancer survivors for an extended period of time [30]. Therefore, the fear of cancer treatment can be another underlying trigger that contributes to more suicidal behaviors among SMN patients. Indeed, in our analysis, we found SMN patients who underwent chemotherapy/radiotherapy or surgery for their FMN had a higher relative risk for suicide death, providing supportive evidence to this notion.

The major merits of our study include the large population-based sample of cancer survivors across the USA and the complete follow-up period, which ensures the presentiveness of the study sample. Also, the large sample size enabled detailed analyses for all subgroups, especially by different follow-up times since diagnosis. The data on cancer diagnosis and cause of death are collected prospectively and independently, which minimizes the risk of information bias. In addition, using the enriched information on tumor characteristics and cancer treatment, we were able to control for important tumor- and treatment-related confounders in our analysis.

Our study has several limitations. First, the misclassification of some causes of death may be a concern. However, it is unlikely that the misclassification would differ substantially between patients with malignancy and the general population. Second, the SEER program merely recruited cancer patients, lacking a cancer-free group as a reference. However, the comparisons of the suicide rates between our study population and the age-, calendar-year-, and sex-matched general population through SMR calculation facilitate the identification of high-risk time window of suicide for timely and effective intervention. Third, due to the lack of information on some potential confounders, such as lifestyle factors, preexisting psychiatric disorders, and history of somatic illness, the residual confounding could be an issue. During analysis, we have made extra efforts by analyzing lifestyle-related cancers (i.e., alcohol- and smoking-related cancers) separately. As such analyses led to comparable estimates, it seems the lifestyle factor did not substantially modify the observed associations. The role of preexisting psychiatric disorders and history of somatic illness need to be assessed in further investigations. However, the calculated E-value suggested that the observed association was unlikely to be entirely explained by the unmeasured confounding. Finally, the generalization of our findings to the entire nation or other populations needs cautions since SEER areas had better case completeness, greater economic disadvantage, and greater minority diversity than non-SEER areas [31]. Despite these discrepancies, we assume these factors should have a limited effect on the studied association as we compared individuals with FMN to those with SMN in our study, all of which come from SEER areas.

In conclusion, this population-based cohort in the USA indicated that cancer survivors receiving a SMN diagnosis were at an increased risk of suicide, compared with either patients with FMN or the general population. The excess risk was most pronounced within the time period immediately after the SMN diagnosis, highlighting the necessity of providing timely psychological support to patients suffering SMN.

Acknowledgments

The authors acknowledge the efforts of the Surveillance, Epidemiology, and End Results (SEER) Program tumor registries in the creation of the SEER-based database. This work was supported by the National Natural Science Foundation of China (grant no. 81971262 to HS), 1.3.5 project for disciplines of excellence, West China Hospital, Sichuan University (grant no. ZYYC21005 to HS), and Project Grant from Science and Technology Department of Sichuan Providence (grant no. 2020YFS0575 to HS).

Contributor Information

Donghao Lu, Email: donghao.lu@ki.se.

Huan Song, Email: songhuan@wchscu.cn.

Data Availability

The data analyzed in this study were obtained from the Surveillance, Epidemiology, and End Results Program (https://seer.cancer.gov/).

Ethical Approval

This study was approved by the Biomedical Research Ethics Committee of West China Hospital (2020.393).

Disclosure

Part of this work was presented as an oral presentation at the World Congress of Epidemiology on 3–6 September 2021.

Conflicts of Interest

The authors declare that there are no potential conflicts of interest.

Authors' Contributions

DL, HS, and HY were responsible for the study's concept and design. YQ did the project management. HY, CW, and JW did the data cleaning and analysis. HY, DL, and HS interpreted the data. HY, DL, and HS drafted the manuscript. YS did the language edits. All the authors approved the final manuscript as submitted and agree to be accountable for all aspects of the work.

Supplementary Materials

Supplementary Materials

Supplementary Table 1: International Classification of Disease Oncology (ICD-O) third version codes for diagnoses used in this study. Supplementary Table 2: change of the suicide standardized mortality ratios (SMRs) over follow-up periods among patients with first malignant neoplasm (FMN) or second malignant neoplasm (SMN), compared with the general population. Supplementary Table 3: sensitive analysis of the risk of suicide among individuals with a second malignant neoplasm (SMN) diagnosis, by excluding SMN patients with a prior history of first malignant neoplasm (FMN) at the same tumor site (N = 40,076), compared with individuals with FMN.

Click here for additional data file. (28.5KB, docx)

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Associated Data

This section collects any data citations, data availability statements, or supplementary materials included in this article.

Supplementary Materials

Supplementary Materials

Supplementary Table 1: International Classification of Disease Oncology (ICD-O) third version codes for diagnoses used in this study. Supplementary Table 2: change of the suicide standardized mortality ratios (SMRs) over follow-up periods among patients with first malignant neoplasm (FMN) or second malignant neoplasm (SMN), compared with the general population. Supplementary Table 3: sensitive analysis of the risk of suicide among individuals with a second malignant neoplasm (SMN) diagnosis, by excluding SMN patients with a prior history of first malignant neoplasm (FMN) at the same tumor site (N = 40,076), compared with individuals with FMN.

Click here for additional data file. (28.5KB, docx)

Data Availability Statement

The data analyzed in this study were obtained from the Surveillance, Epidemiology, and End Results Program (https://seer.cancer.gov/).

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