Cause-specific mortality and second cancer incidence after non-Hodgkin lymphoma: a report from the Childhood Cancer Survivor Study

Elizabeth C Bluhm; Cécile Ronckers; Robert J Hayashi; Joseph P Neglia; Ann C Mertens; Marilyn Stovall; Anna T Meadows; Pauline A Mitby; John A Whitton; Sue Hammond; Joseph D Barker; Sarah S Donaldson; Leslie L Robison; Peter D Inskip

doi:10.1182/blood-2007-08-106021

. 2008 Feb 7;111(8):4014–4021. doi: 10.1182/blood-2007-08-106021

Cause-specific mortality and second cancer incidence after non-Hodgkin lymphoma: a report from the Childhood Cancer Survivor Study

Elizabeth C Bluhm ^1,^✉, Cécile Ronckers ^1,², Robert J Hayashi ³, Joseph P Neglia ⁴, Ann C Mertens ⁵, Marilyn Stovall ⁶, Anna T Meadows ⁷, Pauline A Mitby ⁴, John A Whitton ⁸, Sue Hammond ⁹, Joseph D Barker ¹⁰, Sarah S Donaldson ¹¹, Leslie L Robison ¹², Peter D Inskip ¹

PMCID: PMC2288716 PMID: 18258798

Abstract

Second primary malignancies and premature death are a concern for patients surviving treatment for childhood lymphomas. We assessed mortality and second malignant neoplasms (SMNs) among 1082 5-year survivors of non-Hodgkin lymphoma (NHL) in the Childhood Cancer Survivor Study, a multi-institutional North American retrospective cohort study of cancer survivors diagnosed from 1970 to 1986. Standardized mortality ratios (SMRs) and standardized incidence ratios (SIRs) were calculated using US population rates. Relative risks for death and solid tumor SMNs were calculated based on demographic, clinical, and treatment characteristics using Poisson regression models. There were 87 observed deaths (SMR = 4.2; 95% CI, 1.8-4.1) with elevated rates of death from solid tumors, leukemia, cardiac disease, and pneumonia. Risk for death remained elevated beyond 20 years after NHL. Risk factors for death from causes other than NHL included female sex (rate ratio [RR] = 3.4) and cardiac radiation therapy exposure (RR = 1.9). There were 27 solid tumor SMNs (SIR = 3.9; 95% CI, 2.6-5.7) with 3% cumulative incidence between 5 and 20 years after NHL diagnosis. Risk factors were female sex (RR = 3.1), mediastinal NHL disease (RR = 5.2), and breast irradiation (RR = 4.3). Survivors of childhood NHL, particularly those treated with chest RT, are at continued increased risk of early mortality and solid tumor SMNs.

Introduction

Non-Hodgkin lymphoma (NHL) accounts for 6% of cancers before age 20 years in the United States.¹ Incidence increases from 0.5 per million at age younger than 5 years to 36.6 per million at ages 15 to 19 years in the United States.² With 5-year survival estimated as 78% for children diagnosed with NHL during 1992 to 1998,³ the increasing number of patients surviving into middle age and late adulthood has prompted concern for adverse late health effects.⁴

Systemic chemotherapy (CT) is the mainstay of treatment for NHL,^5–7 guided by histology and stage.⁸ Despite the ongoing evolution of treatment regimens, studies examining delayed health effects must take into account earlier regimens, including radiation therapy (RT) to bulk disease sites,⁵ central nervous system RT, COMP (cyclophosphamide, vincristine, methotrexate, and prednisone), a leukemia-adapted regimen,⁹ epipodophyllotoxins,¹⁰ doxorubicin, intrathecal CT, and other CT agents, some of which have been associated with second malignancies.^7,11–14 An appreciation of factors associated with impaired long-term survival of these patients will aid clinicians in surveillance of childhood NHL survivors.

Predictors of late mortality and life-threatening late disease are not well established for 5-year survivors of pediatric NHL.^10,15–17 An increased incidence of leukemia and several solid tumors^18–27 as well as cardiomyopathy^28–31 was documented in large studies after treatment for NHL in adulthood. The current analysis was undertaken to provide a detailed assessment of survival, cause-specific mortality, and second cancer incidence among 5-year survivors of NHL in the Childhood Cancer Survivor Study (CCSS) as a reference for healthcare providers monitoring survivors of childhood NHL. The CCSS study population, reflecting a large and unique resource, has been the source of a number of scientific publications.³² Previous reports have addressed outcomes relating to late mortality and second cancers in the entire cohort and after several childhood cancer diagnoses. The current report provides results of detailed analyses, using updated data, to provide a more comprehensive assessment of outcomes in an important subgroup of childhood cancer survivors.

Methods

Study population

Subjects with a confirmed diagnosis of NHL in the years 1970 to 1986 were identified through the CCSS, a multi-institutional retrospective cohort study of children diagnosed with cancer before age 21 who survived 5 years from diagnosis (Document S1, available on the Blood website; see the Supplemental Materials link at the top of the online article). The overall study design has been described previously.³² For the current analyses, eligibility was limited to subjects with a primary diagnosis of NHL (ICD-O-2 codes 9592.3-9723.3). Of 1532 eligible NHL survivors, 1082 (71%) were enrolled on completing a survey questionnaire.

The human subjects committee at each participating institution reviewed and approved the CCSS protocol and questionnaire. Study subjects or parents (if study subject was < 18 years of age at contact) gave written informed consent to participate in the study and for release of medical records in accordance with the Declaration of Helsinki. Subjects were mailed a questionnaire requesting information on demographic characteristics, health practices, and medical conditions. Study questionnaires and medical records abstraction forms are available at www.stjude.org/ccss.

Using ICD-O site and morphology codes, primary site of disease was categorized as lymph nodes/hematopoietic (hereafter referred to as lymph nodes), gastrointestinal, head/neck (including brain), bone, mediastinum/heart (hereafter referred to as mediastinum), unknown, or other sites. NHL histopathology was characterized as Burkitt or Burkitt-like (hereafter referred to as Burkitt); lymphoblastic, including small lymphocytic or small cleaved cell (hereafter referred to as lymphoblastic); diffuse large cell, including immunoblastic, lymphosarcoma and reticulosarcoma (hereafter referred to as diffuse large cell); or other specified or unspecified. Stage information was limited to an assessment of metastases at the time of diagnosis for 750 of 1082 patients. Medical records of initial NHL treatment were reviewed using a standardized data abstraction protocol for 926 of 977 study subjects who consented to medical records review. Treatment details were missing in 5 of 926 subjects, leaving 921 subjects for analyses of therapy.

Abstracted treatment data included cumulative doses (mg/m²) and routes of administration for 28 CT agents³²; surgical procedures related to NHL bulk disease; bone marrow transplantation; and NHL relapse. From individual patients' radiation records, including diagrams, photographs, treatment plans, daily records, and follow-up notes, collaborating medical physicists determined body regions (brain, head, neck, chest, abdomen, spine, pelvis, limbs, and total body) included in any treatment field. The breasts, heart, and thyroid were considered irradiated if any part were included in a treatment field.

Ascertainment of mortality and second malignant neoplasms

Analyses of mortality among 5-year NHL survivors were based on searches of the National Death Index in 1996 and 2002 for all eligible subjects. Among 1082 study participants, there were 89 confirmed deaths. Eighty-seven subjects with known date of death were included in analyses of all-cause mortality. Underlying cause of death was obtained from 79 death certificates and from 3 families and was not determined for 5 deaths.

Analyses of second malignant neoplasms (SMNs) were based on self-reported questionnaire responses through December 31, 2002, with review by study pathologist. Only second, and not third or subsequent, malignancies were included in analyses. SMNs that arose less than 5 years after initial NHL diagnosis date were not included. In cases in which the SMN could have represented recurrence of the original condition, the pathology reports were compared and slides were requested for review. If the determination could not be made, a conservative approach was taken and the case was classified as a recurrence.

Statistical analyses

SMRs were calculated as ratios of observed (O) to expected (E) numbers of deaths, calculated based on age-, sex-, and calendar time-specific mortality rates for the United States, obtained from the National Center for Health Statistics. Person-time at risk of mortality in survivors was considered to extend from 5 years after NHL diagnosis until the earliest of the date of death, most recent vital status assessment, or close of study follow-up (December 31, 2002). Excess absolute risks (EARs) were calculated as (O − E)/10 000 person-years.

Standardized incidence ratios (SIRs) were calculated as ratios of observed to expected numbers of new incident cancers, based on incidence rates from the US Surveillance, Epidemiology, and End Results (SEER) population-based cancer registries adjusted for age, sex, race, and calendar time period.³ Person-time at risk for second malignancies lasted from 5 years after NHL diagnosis until the earliest of the date of first SMN diagnosis, death, or most recent follow-up questionnaire, if completed by December 31, 2002. The SEER*Stat program (Information Management Systems, Rockville, MD) was used to calculate SMRs, SIRs, and EARs within strata of demographic, clinical, and treatment characteristics. The cumulative incidence of second cancers, adjusted for competing risks, was computed according to the method of Gooley et al.³³ The Kaplan-Meier method was used to calculate proportional survival. Because cumulative incidence of SMNs has been calculated in some other studies using the Kaplan-Meier method, which does not adjust for competing risks, we also used this method to enhance comparability between studies. Analyses of SMNs focused on solid cancers arising in organs other than bone marrow or lymph nodes, excluding lymphoma and leukemia.

Poisson regression was used to calculate rate ratios (RRs) for all-cause mortality and solid SMN incidence among NHL survivors.³⁴ Regression analyses were performed using the routine GENMOD (SAS version 9.1.3; SAS Institute, Cary, NC) incorporating external reference rates from SEER registries. Cohort members without medical records abstraction were excluded from analyses of therapeutic exposures; however, they contributed to analyses of demographic and disease characteristics. Variables examined for potential confounding or effect modification included age at NHL diagnosis, calendar year of NHL diagnosis, sex, race/ethnicity, and smoking. Likelihood ratio tests were conducted using 2-sided P values, and 95% likelihood-based confidence intervals (CIs) were calculated. Regression analyses were performed using SAS PROC PHREG (SAS Institute).

Results

Study subjects who were 5-year survivors of pediatric NHL were 70% male and 86% non-Hispanic white (Table 1). The median age at NHL diagnosis was 10 years. For mortality analyses, follow-up ranged from 0 to 27 years (mean, 17 years) from eligibility to death or the study close. Predominant lymphoma subtypes were Burkitt, lymphoblastic, and diffuse large cell, and the most common location was in lymph nodes (Table 1).

Table 1.

Demographic, clinical, and treatment characteristics of 1082 five-year survivors of pediatric non-Hodgkin lymphoma (NHL): Childhood Cancer Survivor Study, North America

	No. (%)
Sex
Male	762 (70)
Female	320 (30)
Race/ethnicity
White non-Hispanic	935 (86)
Black	46 (4)
Other	95 (9)
Missing	6 (1)
Age at NHL diagnosis, y
≤4	184 (17)
5-9	326 (30)
10-14	346 (32)
15-21	226 (21)
Attained age at death or at close of study, years^*
<20	33 (3)
20-29	364 (34)
30-39	518 (48)
≥40	165 (15)
NHL histopathology or cell type^†
Burkitt/Burkitt-like (9686.3, 9687.3)	245 (23)
Lymphoblastic (9685.3) and small cell (9670.3, 9672.3)	244 (23)
Diffuse large cell (9680.3-9684.3, 9592.3, 9593.3)	218 (20)
Other histopathology or cell types, specified	142 (13)
Histiocytosis (9720.3, 9723.3)	52 (5)
Follicular and nodular NHL (9690.3-9698.3)	45 (4)
Mixed-cell type (9675.3)	10 (1)
Others (9593.3, 9702.3, 9704.3, 9709.3, 9714.3)	35 (3)
Unspecified cell type (9590.3, 9591.3)	233 (22)
Stage at NHL diagnosis
Not metastatic	482 (45)
Metastatic	268 (25)
Unknown/missing	332 (31)
Site of primary NHL
Lymph nodes	523 (48)
Gastrointestinal tract	109 (10)
Head and neck, including brain	122 (11)
Mediastinum or heart	81 (7)
Bone	52 (5)
Other sites	140 (13)
Unknown	55 (5)
Year of NHL diagnosis
1970-1973	122 (11)
1974-1977	211 (20)
1978-1981	311 (29)
1982-1986	438 (40)
Treatment regimens
CT, no RT	276 (25)
RT, no CT	37 (3)
Both RT and CT	596 (55)
Neither RT nor CT	12 (1)
Missing data on either CT or RT	2 (<1)
Missing all treatment data	159 (15)
Bone marrow transplantation
No	1033 (95)
Yes	29 (3)
Unknown/missing	20 (2)

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CT indicates chemotherapy; and RT, radiation therapy.

Age as of December 31, 2002, for subjects alive on that date; excludes two with unknown date of death.

^†

By ICD-O-2 code.

The proportion of subjects receiving CT rose from 67% to 95% during the study years 1970 to 1986, whereas RT declined from 85% to 53%. The proportion receiving 35 Gy or higher maximum tumor dose declined from 48% to 11%. Overall, 65% received combination CT and RT and 30% received CT only. More than 70% of all subjects received COMP. Doxorubicin and bleomycin were used more in older children (age, 15-20 years) with diffuse large cell lymphoma. Epipodophyllotoxins were used more often for lymphoblastic lymphoma than overall (17% vs 9%).

During 18 261 person-years of follow-up, 87 deaths occurred at a median age of 24 years and a median of 13 years after NHL diagnosis. Death occurred 4 times more often than expected among NHL survivors (SMR = 4.2; EAR = 36.3/10 000 person-years) (Table 2), with a higher SMR in female (SMR = 8.1; 95% CI, 5.3-12.0) than male (SMR = 3.5; 95% CI, 2.7-4.4) subjects. The cause-specific mortality rate ratio and difference were elevated for death from NHL, leukemia, solid tumors, cardiac diseases (primarily cardiomyopathy), and pneumonia, but not from external causes, including accidents, suicide, and homicide. The mortality rate ratio for death from all causes was highest 5 to 9 years after NHL diagnosis and was largely attributable to NHL deaths. Observed deaths remained higher than expected 20 or more years from NHL diagnosis for mortality from NHL, solid tumor SMNs, and cardiac diseases. Absolute risk (EAR) of death from circulatory disease increased with time since diagnosis. EAR for death from NHL declined and then later rose with increasing time since diagnosis. EARs for death from solid tumors were first significantly elevated 10 years from NHL diagnosis and remained relatively constant. There was only 1 death from a solid tumor within years 5 to 10. EARs for death from any cause declined and then increased with increasing time since diagnosis. Among 5-year survivors, proportional survival at 20 years after NHL diagnosis was 0.91.

Table 2.

Observed (O) and expected (E) numbers of deaths, and overall and cause-specific standardized mortality ratios (SMR) and excess absolute risks (EAR) among 1082 five-year survivors of pediatric non-Hodgkin lymphoma (NHL): Childhood Cancer Survivor Study, North America

Cause of death (ICD-9)	Years after NHL diagnosis
	5-9			10-19			At least 20			Total at least 5 years from diagnosis
	O	SMR (95% CI)	EAR	O	SMR (95% CI)	EAR	O	SMR (95% CI)	EAR	O	E	SMR (95% CI)	EAR
All causes	32	7.1 (4.9, 10.0)	52.1	32	2.9 (2.0, 4.1)	21.9	23	4.2 (2.7, 6.4)	52.7	87	20.9	4.2 (3.3, 5.1)	36.3
All cancers	24	87.2 (55.9, 130)	45.0	15	18.6 (10.4, 30.7)	14.8	9	12.5 (5.7, 23.8)	24.8	48	1.8	26.7 (19.7, 35.4)	25.4
Lymphopoietic and hematopoietic
Non-Hodgkin lymphoma^*	23	188.1 (119, 282)	43.4	5	19.2 (6.2, 44.8)	4.9	3	23.7 (4.8, 69.1)	8.6	31	0.5	60.8 (41.3, 86.4)	16.7
Leukemias^†	14	520.6 (284, 874)	26.5	4	49.3 (13.3, 126)	4.1	3	57.4 (11.5, 168)	8.8	21	0.2	131.1 (81.1, 200)	11.4
All solid tumors^‡	9	113.5 (51.8, 216)	16.9	1	—		0	—		10	0.3	37.2 (17.8, 68.4)	5.3
	1	—			18.5 (8.8, 34.0)	9.8	6	10.2 (3.7, 22.3)	16.2	17	1.3	13.3 (7.7, 21.3)	8.6
Circulatory system diseases	2	12.1 (1.4, 43.8)	3.5	3	4.4 (0.9, 12.8)	2.4	7	8.8 (3.5, 18.0)	18.6	12	1.7	7.3 (3.8, 12.7)	5.7
Cerebrovascular disease	1	—		0	—		1	—		2	0.2	8.3 (0.9, 30.0)	1.0
Cardiac disease	1	—		3	5.6 (1.1, 16.4)	2.6	5	7.6 (2.5, 17.8)	13.0	9	1.3	6.9 (3.1, 13.0)	4.2
Cardiomyopathy	1	—		2	20.2 (2.3, 73.0)	2.0	2	25.9 (2.9, 93.6)	5.8	5	0.2	24.8 (8.0, 57.8)	2.6
Other causes of death^§
Pneumonia	1	—		2	20.7 (2.3, 74.8)	2.0	0	—		3	0.2	15.4 (3.1, 45.1)	1.5
Digestive system diseases	0	—		0	—		2	7.9 (0.9, 28.4)	5.2	2	0.5	4.1 (0.5, 14.9)	0.8
External causes of death	2	0.6 (0.1, 2.1)	−2.7	5	0.7 (0.2, 1.6)	−2.2	3	1.3 (0.3, 3.8)	2.2	10	12.9	0.8 (0.4, 1.4)	−1.6
Suicide	1	—		4	2.5 (0.7, 6.3)	2.5	0	—		5	2.9	1.8 (0.6, 4.1)	1.2

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Death ratios are based on 87 deaths among 1080 subjects who completed the baseline questionnaire, excluding 2 with unknown date of death.

O indicates observed number of deaths; SMR, standardized mortality ratio; CI, confidence interval; EAR, excess absolute risk (expressed per 10,000 person-years); E, expected number of deaths; —, SMRs and CIs are presented where there are 2 or more deaths from a particular cause.

Non-Hodgkin lymphoma includes 5 cases with reticulosarcoma or lymphosarcoma (ICD-9 2000–2009) and 16 cases with other lymphomas

^†

Leukemias include 6 acute lymphoblastic leukemias (ICD-9=2040), 2 acute myeloid leukemias (ICD-9=2050), and 2 unspecified leukemias.

^‡

Sites of fatal solid nonhematologic tumors and numbers observed (in parentheses) include oral cavity and pharynx (2), lung (2), bone (2), connective tissue (2), breast (2), brain (2), colon (1), testis (1), kidney (1), and unspecified (2).

^§

Additional causes of death were systemic sclerosis (1), polymyositis (1), septicemia (1), nonmalignant brain neoplasm (1), alcohol-related (1), other metabolic (1), and other/ill-defined (1).

Female sex, cardiac RT exposure, doxorubicin, and bleomycin were associated with increased relative risk of mortality from causes other than NHL in a multivariate model adjusted for RT and histopathology (Table 3). In a multivariate model including all of these factors, only female sex (RR = 2.8; 95% CI, 1.5-5.1) and cardiac RT exposure (RR = 2.1; 95% CI, 1.1-3.9) retained significant associations. No excess mortality risk was associated with alkylating agents as a group or with exposure to daunorubicin, cyclophosphamide, ifosfamide, hydroxyurea, methotrexate, vincristine, steroids, 6-mercaptopurine, L-asparaginase, 6-thioguanine, carmustine, or surgical procedures. Treatment with Ara-C, doxorubicin, epipodophyllotoxins, bleomycin, platinum drugs, and bone marrow transplantation was associated with an increased mortality rate ratio for deaths attributable to NHL (Table 3). No excess risk was associated with RT to the total body, abdomen, pelvis, brain, neck, spine, or limb. Cardiac RT exposure was nonsignificantly associated with death from cardiac diseases (RR = 4.6; 95% CI, 0.9-33.2). Of 3 deaths from pneumonia, 2 bacterial pneumonias occurred in subjects with history of splenectomy and 1 viral pneumonia occurred in a subject without history of splenectomy. During the later study years, there was a suggestion of a decreasing RR for causes other than NHL; however, this trend did not reach statistical significance (P =.098).

Table 3.

All-cause mortality and risk of death relative to demographic, clinical, and treatment-related factors among 1080 five-year survivors of pediatric non-Hodgkin lymphoma (NHL): Childhood Cancer Survivor Study, North America

	Total	Deaths from NHL, n = 21		Deaths from other causes, n = 66
	Total	O	RR (95% CI)	O	RR (95% CI)
Sex
Male	760	18	1.0	44	1.0
Female	320	3	0.3 (0.01, 1.3)	22	3.4 (1.9, 5.9)
Age at NHL diagnosis, y
0-4	184	3	1.0	7	1.0
5-9	325	3	0.7 (0.2, 2.2)	19	1.0 (0.4, 3.1)
10-14	346	7	0.6 (0.1, 2.2)	20	1.0 (0.4, 3.2)
15-21	225	8	2.0 (0.4, 6.9)	20	0.9 (0.4, 2.9)
Year of NHL diagnosis
1970-1973	122	8	1.2 (0.4, 4.8)	20	1.9 (0.8, 4.7)
1974-1977	211	1	0.2 (0.01, 1.2)	16	1.4 (0.6, 3.3)
1978-1981	310	7	1.1 (0.3, 4.2)	18	1.1 (0.5, 2.8)
1982-1986	437	5	1.0	12	1.0
					P trend=.098
NHL histopathology or cell type
Burkitt/Burkitt-like	245	1	1.0	7	1.0
Lymphoblastic	243	5	3.8 (0.6, 74.0)	17	2.3 (0.8, 7.1)
Diffuse large cell	217	7	5.2 (0.9, 96.9)	15	2.0 (0.8, 6.2)
Others, specified	142	3	2.4 (0.2, 51.0)	12	2.0 (0.6, 6.7)
Unspecified	233	5	4.0 (0.6, 76.4)	15	1.9 (0.7, 6.0)
Treatment exposures^*
Any RT	633	17	2.5 (0.7, 16.1)	45	1.7 (0.8, 3.9)
Cardiac exposure to RT	122	6	1.8 (0.6, 4.8)	15	1.9 (1.0, 3.6)
Any CT	870	16	1.4 (0.4, 8.9)	50	1.1 (0.5, 3.2)
COMP	668	13	Unable	34	1.1 (0.4, 3.2)
Ara-C	411	12	5.0 (1.9, 14.8)	25	1.4 (0.7, 2.4)
Doxorubicin	293	10	4.0 (1.6, 10.6)	21	1.8 (1.0, 3.1)
Epipodophyllotoxins	83	6	9.4 (3.1, 25.6)	7	1.5 (0.5, 3.6)
Bleomycin	56	8	14.5 (5.4, 38.2)	7	2.4 (1.0, 5.0)
Platinum compounds	14	5	85.6 (26.1, 242)	2	4.7 (0.8, 16.0)
Bone marrow transplantation	26	3	10.0 (2.2, 31.8)	3	2.7 (0.7, 7.5)

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Results are based on demographic data presented for 1080 subjects who completed the baseline questionnaire, excluding two with unknown date of death.

O indicates observed; RR, rate ratio (based on Poisson regression); analyses are adjusted for sex and RT exposure.

Treatment data were available for 921 subjects, including 73 of 87 deaths. RT, radiation therapy; CT, chemotherapy; COMP, cyclophosphamide, vincristine, methotrexate, and prednisone. The referent group for each treatment exposure consists of subjects who did not receive that treatment. Treatment results are adjusted for NHL and histopathology. CT and BMT results are additionally adjusted for RT.

There were 31 self-reported and histologically confirmed malignant cancers among 5-year survivors, including 27 solid tumor malignancies, 3 lymphomas, and 1 leukemia (Table 4). The incidence of new malignancies was more than 3 times the expected rate (SIR = 3.5; 95% CI, 2.5-4.0) with significant excesses of cancer of the breast, thyroid, oral cavity and pharynx, bone, brain, and bladder. Figure 1 presents the cumulative incidence for second malignancies and other nonmalignant second tumors beyond 5 years from NHL diagnosis.

Table 4.

Observed (O) and expected (E) cancer incidence and standardized incidence ratios (SIR) among 1082 five-year survivors of pediatric non-Hodgkin lymphoma (NHL): Childhood Cancer Survivor Study, North America

Incident second cancer	Self-reported second cancer				Self-reported second cancer and cancer cases identified on death certificates^*
Incident second cancer	O	E	SIR (95% CI)	EAR	O	SIR (95% CI)
Any malignancy^†	31	8.9	3.5 (2.4, 5.0)	13.1	34	3.8 (2.7, 5.4)
Lymphomas and hematopoietic cancer
Lymphoma	3	1.4	2.1 (0.4, 6.2)	0.9	3	2.1 (0.4, 6.2)
NHL	1	0.7	ND	0.2	1	ND
Hodgkin lymphoma	2	0.7	2.8 (0.3, 10.1)	0.8	2	2.8 (0.3, 10.1)
Leukemia	1	0.5	ND	0.3	3	6.5 (1.3, 18.9)
Any solid nonhematologic tumor	27	6.9	3.9 (2.6, 5.7)	11.9	28	4.1 (2.7, 5.9)
Breast	6	0.7	9.1 (3.3, 19.7)	3.2	6	9.1 (3.3, 19.7)
Thyroid	6	0.6	9.4 (3.5, 20.5)	3.2	6	9.4 (3.5, 20.5)
Oral cavity and pharynx	3	0.2	14.4 (2.9, 42.1)	1.7	3	14.4 (2.9, 42.1)
Bones and joints	2	0.2	11.6 (1.3, 41.8)	1.1	2	11.6 (1.3, 41.8)
Brain and nervous system	3	0.5	5.8 (1.2, 16.8)	1.5	4	7.7 (2.1, 19.7)
Urinary bladder	2	0.1	14.5 (1.6, 52.2)	1.1	2	14.5 (1.6, 52.2)
Others	5^‡	ND	ND	ND	5^‡	ND

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O indicates observed number of cancers; E, expected number of cancers; SIR, standardized incidence ratio; CI, confidence interval; EAR, excess absolute risks (expressed per 10,000 person-years); ND, not determined (estimates presented where there are two or more observed cancers).

For deceased study participants whose family member filled out the study questionnaire, there were three cases in which a SMN was not reported but was present on the death certificate and where the date of death preceded the last questionnaire. Cases included one cranial nerve neoplasm and two acute myeloid leukemias.

^†

Excluded were: five cancers reported less than five years after NHL diagnosis: fibrillary astrocytoma, osteosarcoma of bone/joint, sarcoma of bone/joint, salivary gland carcinoma, and lymphoblastic lymphoma; two incident third malignancies: cancer of the parotid gland after papillary thyroid cancer, and renal cell carcinoma after endometrial cancer; four cancer diagnoses identified on death certificates but not on a subsequent questionnaire: two AMLs and two brain cancers, four meningiomas, one myelodysplastic syndrome, and 49 non-melanoma skin cancers in 24 individuals.

^‡

One solid tumor occurred at each of the following sites: colon, skin (melanoma), uterus, vulva, and testis.

**Cumulative incidence of second neoplasms among 1074 5-year survivors of pediatric non-Hodgkin lymphoma, Childhood Cancer Survivor Study, North America**. The dashed line represents cumulative incidence of all malignant diagnoses, including bladder transitional cell carcinoma in situ, whereas the solid line includes diagnoses listed above in addition to 4 meningiomas (ICD-O-2: 9532.0, 953.0), 21 skin cancers (ICD-O-2: 8090.3, 8094.3), and one myelodysplastic syndrome (ICD-O-2: 9989.1). Only the first of any of these neoplasms is counted for each subject. Subjects were those alive 5 years after NHL diagnosis, excluding 6 who experienced secondary neoplasms within the first 5 years of NHL and 2 with unknown date of death.

The SIR for solid tumor SMNs was higher in female than male subjects (Table 5) and remained significantly elevated in women after excluding breast cancer (SIR = 6.4; 95% CI, 3.3-11.1). Five of 6 thyroid cancer SMNs occurred in women, including 4 papillary carcinomas. One case of infiltrating ductal carcinoma of the breast was diagnosed in a man. No solid tumor SMNs were diagnosed after Burkitt lymphoma or NHL diagnosis before the age of 5 years. The SIR for solid tumor SMNs was significantly elevated for attained ages 5 to 19, 20 to 29, and 30 to 39 years. Overall cumulative incidence of solid tumor SMNs from 5 to 20 years after NHL diagnosis was 0.03 (95% CI, 0.02-0.05).

Table 5.

Standardized incidence ratios and relative risks for solid second malignant neoplasms by demographic and disease characteristics and by type of treatment among 1082 five-year survivors of pediatric non-Hodgkin lymphoma (NHL): Childhood Cancer Survivor Study, North America

	All solid malignancies, n = 27
	O	SIR (95% CI)	RR (95% CI)
Overall risk	27	3.9 (2.6, 5.7)	NA
Sex
Male	10	2.3 (1.1, 4.3)	1.0
Female	17	6.8 (3.9, 10.8)	2.2 (1.0, 5.2)
Age at NHL diagnosis, y
0-4	1
5-9	5	3.6 (1.2, 8.4)	1.1 (0.3, 3.4)
10-14	12	5.2 (2.7, 9.0)	1.8 (0.7, 4.6)
15-21	9	3.4 (1.5, 6.4)	1.0
NHL treatment era
1970-1973	5	3.2 (1.0, 7.6)	1.0
1974-1977	4	2.0 (0.5, 5.1)	1.0 (0.2, 4.9)
1978-1981	10	5.4 (2.6, 9.8)	2.8 (0.8, 12.4)
1982-1986	8	5.6 (2.4, 11.1)	2.8 (0.8, 13.2)
			P trend = .032
NHL histopathology or cell type
Burkitt/Burkitt-like	0	0 (0, 3.0)	ND
Lymphoblastic	6	4.6 (1.7, 10.0)	1.5 (0.4, 6.0)
Diffuse large cell	10	5.4 (2.6, 10.0)	1.9 (0.6, 7.0)
Others specified	6	6.3 (2.3, 13.7)	1.7 (0.4, 7.3)
Unspecified	5	3.3 (1.1, 7.7)	1.0
Primary site of NHL
LN/hematopoietic	10	3.0 (2.9, 7.1)	1.0
GI	1	ND	ND
Head and neck, including brain	2	3.0 (0.3, 10.8)	0.6 (0.3, 3.0)
Mediastinum	7	14.6 (5.8, 30.0)	4.6 (1.6, 12.5)
Unknown primary/others	7	5.7 (2.3, 11.8)	1.8 (0.6, 5.0)
Treatment exposures^*
Any RT	21	4.7 (2.9, 7.1)	2.1 (0.9, 4.8)
Breast exposure to RT^†	12	11.8 (6.1, 20.6)	7.5 (2.6, 26.7)
Thyroid exposure to RT	10	7.4 (3.5, 13.5)	2.6 (1.0, 7.1)
Any CT	24	4.6 (2.9, 6.8)	Unable
COMP	18	4.9 (2.9, 7.8)	Unable
Ara-C	13	6.0 (3.2, 10.2)	2.4 (1.0, 5.6)
Doxorubicin	9	5.4 (2.4, 10.2)	1.6 (0.7, 3.7)
Epipodophyllotoxins	2	5.4 (0.6, 19.4)	1.2 (0.2, 4.2)
Bleomycin	2	4.8 (0.5, 17.4)	0.9 (0.1, 3.2)
Platinum drugs	1	ND	4.6 (0.3, 23.5)
Bone marrow transplantation	2	14.9 (1.7, 53.8)	3.6 (0.6, 112.5)

Open in a new tab

O indicates observed; SIR, standardized incidence ratio; CI, confidence interval; RR, rate ratio, based on Poisson regression (RR analyses adjusted for RT and sex); NA, not applicable; ND, not determined.

RT, radiation therapy; CT, chemotherapy; COMP, cyclophosphamide, vincristine, methotrexate, and prednisone. Referent in each drug/regimen is all subjects unexposed to that drug/regimen. Treatment results are adjusted for NHL pathology and sex. CT and BMT results are additionally adjusted for RT.

^†

Breast exposure includes shielded breast exposure. Because of sparse data, model for breast exposure did not account for gastrointestinal tract of head and neck sites.

In a Poisson regression model adjusted for any RT and sex, female sex and mediastinal site of NHL were significantly associated with solid tumor SMNs. There was a trend to increasing SMN diagnosis among patients treated in more recent years (P trend = .032). The only CT agent significantly associated with solid tumor SMNs was Ara-C (Table 5). Shielded or unshielded breast exposure to RT was associated with a 7-fold increased risk of solid tumor SMNs, and exposure of the thyroid was associated with a more than 2-fold increased risk. RT involving the total body, abdomen, pelvis, brain, spine, or limb was not significantly associated with solid SMNs. In a multivariate model, female sex, mediastinal disease, and breast RT remained associated with solid tumor SMNs. Sensitivity analyses including 3 additional cancers ascertained from death certificates (where death occurred before the last questionnaire, which was completed by a family member) did not yield a meaningful change in SIR or RR estimates.

Discussion

Our findings among a cohort of 1082 five-year NHL survivors in the CCSS indicate a 3-fold overall risk of SMNs and 4-fold risk of mortality relative to the general U.S. population. There were higher than expected SMRs for death from NHL, solid tumor SMNs, leukemia, cardiac disease, and pneumonia. There was a higher than expected relative risk of death from causes other than NHL in female subjects and after cardiac RT exposure. Despite the higher relative risk of SMNs among patients diagnosed in the later vs earlier years of the 1970 to 1986 study period, the RR of death was not increased in later years, perhaps indicating advances in survival from some treatment-related late effects.

All-cause mortality after NHL was lower than among 5-year survivors of other childhood cancers followed in the CCSS through 1996.³⁵ Our study extends follow-up of NHL diagnoses through the end of 2002 and incorporates primary NHL histopathology categories. We found elevated death rates from second cancers and cardiac and pulmonary diseases, particularly cardiomyopathy and pneumonia, as has been seen after other childhood cancers^35–37 and after adult NHL treatment.^28–31 The increased risk of death associated with chest RT suggests that NHL treatment may convey some risks similar to those seen after Hodgkin's lymphoma.³⁸ Based on a small number of cases in our cohort, death from nonviral pneumonia occurred only after splenectomy. Our finding of increased risk of death from causes other than NHL among female subjects is consistent with sex-specific differences in anthracycline-associated cardiac damage and certain other health conditions reviewed by Armstrong et al.³⁹ Similarly, in a Nordic population-based study of 13 711 five-year survivors of 13 pediatric cancers, including 781 NHL survivors, the all-cause mortality was significantly higher in females than in males.⁴⁰ However, no SMR estimates were provided by sex or treatment risk factors for NHL patients specifically as in our study. Despite seeing only 87 deaths in our cohort, our data raise the possibility that 5-year survivors of NHL appear to remain at considerable risk of death from NHL even years after diagnosis.

We focused on solid tumor SMNs as the primary type of SMN seen among 5-year survivors and as pathologically distinct from NHL recurrence. Risk factors associated with solid tumor SMNs in our study population were female sex and thoracic exposure to RT. Four prior publications have reported SIRs between 3.9 and 12 for SMNs after pediatric NHL.^10,41–44 Higher SIRs were seen in an analysis of 456 French and British 3-year survivors of pediatric NHL⁴⁴ and in a St Jude study of SMNs occurring after NHL diagnosis among 497 pediatric NHL patients.¹⁰ Both studies included neoplasms diagnosed within the first 5 years, and allowed lymphoma⁴⁴ or lymphoma and leukemia¹⁰ diagnoses to be counted, probably raising the SIRs. Analyses in the US SEER cancer registry indicated a nearly 4-fold (SIR = 3.9) significantly elevated risk of solid tumor SMNs after NHL diagnosis before the age of 18 years, beginning 2 months after NHL diagnosis.⁴² With extended follow-up in the registry, SIR was 5.3 for all SMNs after NHL diagnosis.⁴³ The SIRs reported after pediatric NHL are higher than after adult NHL, for which SIR estimates for all SMNs range from 0.9 to 1.6,^19,20,22,27 and demonstrate a decline with increasing age at NHL diagnosis.^18,20

The SIR was increased for solid tumor SMNs at all attained ages from 5 to 39 years. The mean age of living NHL survivors in our study population was only 32.5 years on December 31, 2002, and risks at older ages cannot be directly predicted from these data. Persistently elevated SMRs more than 20 years after diagnosis are concerning and should be confirmed when cohorts of pediatric NHL survivors reach later adulthood. With the evolution of treatments for pediatric NHL and decreasing use of RT, we anticipate changes in the incidence of severe or life-threatening late effects.

Limitations of the current study include the possibility that some associations may have resulted from chance, given small numbers of deaths and second cancers. However, there are few available large populations in which to estimate cumulative and RRs of SMNs after rare childhood cancer diagnosis. Self-reporting of SMNs via periodic mailed questionnaires may underestimate SMN incidence; however, we found no meaningful change in SIRs or RRs for solid tumor SMNs by including additional cancers ascertained from death certificates. Another limitation, restricting study eligibility to 5-year survivors, prevented evaluation of therapy-related leukemia, which more often occurs within the first 5 years of diagnosis. For analyses of RT effects, our study did not calculate absorbed dose to regions of interest or incorporate scatter from nearby treatment areas. Lastly, whereas we included only second primary cancers, the SEER data with which our observed cases were compared included third and subsequent cancers, possibly leading us to underestimate the relative incidence of SMNs in NHL survivors.

The strength of our findings derives from the comparatively large cohort of children with NHL and detailed treatment information available from medical records using the unique resource of the CCSS. We add to a small literature reporting SMRs, SIRs, and predictors of death and SMNs after pediatric NHL. Separate analyses of relative risks for death from NHL and from other causes distinguishes the adverse effects of therapies from the high risk of death in subjects receiving aggressive regimens. Persistently elevated mortality rates beyond 20 years after NHL diagnosis suggests that healthcare providers responsible for this high-risk population should remain alert to second cancers and cardiac disease among long-term survivors, particularly women and those treated with chest RT. Future studies in the CCSS cohort and in aging populations of pediatric NHL survivors are needed to assess additional nonfatal age-related conditions.

Supplementary Material

[Supplemental Appendix]

blood_blood-2007-08-106021_index.html^{(1.1KB, html)}

Acknowledgments

The authors thank the Childhood Cancer Survivor Study institutions and investigators for their participation in this study. The authors thank Jeremy Miller of Information Management Systems for data preparation.

This work was supported by the NCI (grant U24 CA55727, L.L.R., Principal Investigator), the University of Minnesota from the Children's Cancer Research Fund, and St Jude Children's Research Hospital from the American Lebanese Syrian Associated Charities; and by the Intramural Research Program of the NIH, NCI, Division of Cancer Epidemiology and Genetics.

The content of this publication does not necessarily reflect the views or policies of the Department of Health and Human Services, nor does mention of trade names, commercial products, or organizations imply endorsement by the US Government.

Footnotes

The online version of this article contains a data supplement.

The publication costs of this article were defrayed in part by page charge payment. Therefore, and solely to indicate this fact, this article is hereby marked “advertisement” in accordance with 18 USC section 1734.

Authorship

Contribution: E.C.B. designed and performed analyses and wrote the paper; P.D.I. and C.R. designed analyses; C.R., R.J.H., P.D.I., S.S.D., and A.T.M. contributed to interpretation of data; C.R., P.D.I., A.T.M., L.L.R., and S.H. edited the paper; J.P.N., M.S., A.C.M., J.A.W., and P.A.M. collected and prepared data; M.S. performed radiation dosimetry analyses; J.D.B. prepared and analyzed data and made the figure; L.L.R. designed the overall CCSS research project.

A complete list of the participating institutions and investigators of the Childhood Cancer Survivor Study can be found in Document S1, available on the Blood website; see the Supplemental Materials link at the top of the online article.

Conflict-of-interest disclosure: The authors declare no competing financial interests.

Correspondence: Elizabeth C. Bluhm, Radiation Epidemiology Branch, Division of Cancer Epidemiology and Genetics, NCI, 6120 Executive Boulevard, MSC 7238, Rockville, MD 20892-7238; e-mail: bluhme@mail.nih.gov.

References

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Associated Data

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

Supplementary Materials

[Supplemental Appendix]

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blood_blood-2007-08-106021_1.pdf^{(26.7KB, pdf)}

[B1] 1.Ries LAG, Smith MA, Gurney JG, et al. Bethesda, MD: National Cancer Institute, SEER Program; 1999. Cancer incidence and survival among children and adolescents: United States SEER program 1975-1999 [National Institutes of Health Publication No. 99–4649]. [Google Scholar]

[B2] 2.O'Leary M, Sheaffer J, Keller F, Shu X-O, Cheson B. Lymphomas and reticuloendothelial neoplasms. In: Bleyer A, O'Leary M, Barr R, Ries LAG, editors. Cancer Epidemiology in Older Adolescents and Young Adults 15 to 29 Years of Age. Including SEER Incidence and Survival: 1975-2000 [National Institutes of Health Publication No. 06–5767] Bethesda, MD: National Cancer Institute; 2006. [Google Scholar]

[B3] 3.Ries LAG, Eisner MP, Kosary CL. Bethesda, MD: National Cancer Institute; SEER Cancer Statistics Review, 1973-1999. p. 2002. [Google Scholar]

[B4] 4.Schwartz CL. Long-term survivors of childhood cancer: the late effects of therapy. Oncologist. 1999;4:45–54. [PubMed] [Google Scholar]

[B5] 5.Magrath IT, Haddy TB, Adde MA. Treatment of patients with high grade non-Hodgkin's lymphomas and central nervous system involvement: is radiation an essential component of therapy? Leuk Lymphoma. 1996;21:99–105. doi: 10.3109/10428199609067586. [DOI] [PubMed] [Google Scholar]

[B6] 6.Weinstein HJ, Tarbell NJ. ed 7. Philadelphia, PA: Lippincott Williams & Wilkins; 2005. Leukemias and Lymphomas of Childhood. [Google Scholar]

[B7] 7.Sandlund JT. Childhood lymphoma. In: Abeloff MD, Armitage JO, Lichter JO, Niederhuber JE, editors. Clinical Oncology. ed 2. New York: Churchill Livingstone; 2000. pp. 2435–2450. [Google Scholar]

[B8] 8.Gross TG, Termuhlen AM. Pediatric non-Hodgkin's lymphoma. Curr Oncol Rep. 2007;9:459–465. doi: 10.1007/s11912-007-0064-6. [DOI] [PubMed] [Google Scholar]

[B9] 9.Anderson JR, Wilson JF, Jenkin DT, et al. Childhood non-Hodgkin's lymphoma: the results of a randomized therapeutic trial comparing a 4-drug regimen (COMP) with a 10-drug regimen (LSA2-L2). N Engl J Med. 1983;308:559–565. doi: 10.1056/NEJM198303103081003. [DOI] [PubMed] [Google Scholar]

[B10] 10.Leung W, Sandlund JT, Hudson MM, et al. Second malignancy after treatment of childhood non-Hodgkin lymphoma. Cancer. 2001;92:1959–1966. doi: 10.1002/1097-0142(20011001)92:7<1959::aid-cncr1715>3.0.co;2-y. [DOI] [PubMed] [Google Scholar]

[B11] 11.Neglia JP, Friedman DL, Yasui Y, et al. Second malignant neoplasms in five-year survivors of childhood cancer: childhood cancer survivor study. J Natl Cancer Inst. 2001;93:618–629. doi: 10.1093/jnci/93.8.618. [DOI] [PubMed] [Google Scholar]

[B12] 12.Bassal M, Mertens AC, Taylor L, et al. Risk of selected subsequent carcinomas in survivors of childhood cancer: a report from the Childhood Cancer Survivor Study. J Clin Oncol. 2006;24:476–483. doi: 10.1200/JCO.2005.02.7235. [DOI] [PubMed] [Google Scholar]

[B13] 13.Garwicz S, Anderson H, Olsen JH, et al. Second malignant neoplasms after cancer in childhood and adolescence: a population-based case-control study in the 5 Nordic countries. The Nordic Society for Pediatric Hematology and Oncology. The Association of the Nordic Cancer Registries. Int J Cancer. 2000;88:672–678. doi: 10.1002/1097-0215(20001115)88:4<672::aid-ijc24>3.0.co;2-n. [DOI] [PubMed] [Google Scholar]

[B14] 14.Hawkins MM, Wilson LM, Burton HS, et al. Radiotherapy, alkylating agents, and risk of bone cancer after childhood cancer. J Natl Cancer Inst. 1996;88:270–278. doi: 10.1093/jnci/88.5.270. [DOI] [PubMed] [Google Scholar]

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PERMALINK

Cause-specific mortality and second cancer incidence after non-Hodgkin lymphoma: a report from the Childhood Cancer Survivor Study

Elizabeth C Bluhm

Cécile Ronckers

Robert J Hayashi

Joseph P Neglia

Ann C Mertens

Marilyn Stovall

Anna T Meadows

Pauline A Mitby

John A Whitton

Sue Hammond

Joseph D Barker

Sarah S Donaldson

Leslie L Robison

Peter D Inskip

Series information

Abstract

Introduction

Methods

Study population

Ascertainment of mortality and second malignant neoplasms

Statistical analyses

Results

Table 1.

Table 2.

Table 3.

Table 4.

Figure 1.

Table 5.

Discussion

Supplementary Material

Acknowledgments

Footnotes

Authorship

References

Associated Data

Supplementary Materials

ACTIONS

PERMALINK

RESOURCES

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