This is a matched case-control study of men enrolled in the MACS, an ongoing natural history cohort study of men who report sex with men. The MACS was established in 1984, enrolling 6972 HIV-infected and HIV-uninfected MSM over 3 recruitment waves (1984–85 (n=4957), 1987–91 (n=665), 2001–03 (n=1350)) across 4 study sites (Los Angeles, Chicago, Baltimore, and Pittsburgh). Behavioral, clinical, and laboratory data including HIV serology tests were collected at semi-annual visits as described (20, 21). Institutional Review Boards at each study site approved the research, and all participants provided written informed consent.

Participants for this study were 532 HIV-seronegative men over age 18 followed between 1984 and 2010 with no pre-existing cancers and ≥ 2 visits with values for immunological parameters. Thirty-two cases with incident virus-associated cancers were identified through a database search of cancer diagnoses among all HIV-seronegative participants in the MACS (n=3408). For cohort assembly, an initial search identified 25 incident virus-associated cancers that were matched 1:20 to 500 controls without cancer for age at endpoint, race, smoking, and calendar period using the MatchIT package in R version 3.2.4. We later identified 7 additional incident cancers and examined whether case-control matching was still balanced after inclusion of these cases; demographics and smoking were still matched (p>0.20) (Table 1), so we included these additional cases to increase precision of the analysis. HIV negative serostatus was confirmed at study visits within 2 years of cancer diagnosis for 29 cases and within 4 to 5 years for 3 cases. Because all cases remained HIV-seronegative during follow-up, HIV RNA viral load assays were performed for only 3 cases; all were below the limit of detection of the assay (<50 copies per ml of plasma).

The MACS public dataset (P23 release) was translated to a local SQL database and used for the analyses. Immunological parameters and clinical characteristics associated with cancer risk factors were censored at 1 year prior to last follow-up visit for both cases and controls to account for a potential lag between clinical diagnosis of incident cancer and date of cancer diagnosis ascertained through registry linkage. CD4 and CD8 T-cell counts, white blood cell (WBC) counts, CD4/CD8 ratios, and, Fibrosis-4 (FIB-4) score (a non-invasive index of liver fibrosis calculated from age, aspartate aminotransferase (AST), alanine aminotransferase (ALT), and platelet count; FIB-4 <1.45 has a negative predictive value of 90% for advanced fibrosis) (22) were summarized as time-varying variables using values nearest to 1 year before last follow-up visit. Nadir values were the lowest value during follow-up. Time-updated smoking was defined as smoking on average more than half a pack per day within last six years of follow-up. Hepatitis C virus (HCV) infection status was determined by positive HCV antibody or RNA test. HBV infection status was determined by positive Hepatitis B surface antigen (HBsAg) or e-antigen (HBeAg), or HBV DNA test.

A total of 32 incident virus-associated cancers with etiologies linked to HPV, EBV, HHV-8, HBV, or HCV diagnosed during the study period were identified using International Classification of Diseases for Oncology, third edition (ICD-O-3) codes. Incident cancers were ascertained continuously during follow-up using cancer registry linkage data, available medical records and death certificates, and self-reported cancer diagnoses (20). After cancers were classified based on anatomical site and histology (20), analyses focused on a composite category, “virus-associated cancers”, comprised of diagnoses associated with infection by HPV (anal cancer and head and neck squamous cell carcinomas (HNSCC)), EBV (Non-Hodgkin lymphoma [NHL] and Hodgkin lymphoma [HL]), HHV-8 (Kaposi sarcoma [KS]), and HBV/HCV (liver cancer). Despite an established oncogenic role of HPV in development of skin SCC (23), skin cancers were excluded from the analysis given potential confounding effects of ultra-violet exposure, which was not ascertained. ICD-O-3 site codes for anal cancers were 21.0–21.8 and 19.9–20.9 based on a prior study in the MACS cohort (21). ICD-O-3 site codes for HNSCC cases were 2.9, 4.9, and 10.2. The NHL cases were B-cell lymphomas (4 diffuse large B-cell lymphomas, 2 follicular lymphomas, 2 malignant lymphomas of skin and unknown site, 1 mantle cell lymphoma, 1 chronic lymphocytic leukemia).

Univariate or bivariate tests were conducted using Wilcoxon Rank-Sum test, paired t-test, Pearson Chi-Square, or analysis of variance (ANOVA) for cohort characteristics by cancer diagnosis and CD4 count nadir. Exploratory analyses of longitudinal data utilized plots of mean values of immunological parameters for cases and controls during last ten years of follow-up. Linear mixed-effects models were fit for longitudinal CD4 and WBC count as continuous dependent variables over the last six years of follow-up to determine the association between incident viral cancer diagnoses with these parameters and their rates of change. Observation time was left-truncated at six years prior to diagnosis because 428 participants (81.8%) had at least 12 semi-annual visits with immunological data, while data coverage became sparser going back further in time (Supplemental Material 1). Log2 transformation was applied to WBC values to improve normality of distributions. Models were adjusted for baseline age (at six years prior to follow-up), race, heavy smoking, FIB-4 >1.45, and time to diagnosis; all models included random intercepts and slopes. Cox regression models were used to calculate adjusted hazard ratios (HR) of incident virus-associated cancer diagnoses associated with time-varying 2-year lagged CD4 cell count and CD4:CD8 ratio, CD4 count-nadir differential, and CD4 count and CD4:CD8 ratio nadirs during follow-up. We used a stepwise approach to evaluate Cox regression models, screening for predictors among these immunological parameters to evaluate their associations with risk. Modeling started with age, race, smoking, and CD4 count, followed by sequentially replacing the CD4 count variable with CD4 nadir, CD4:CD8 ratio, or CD4:CD8 ratio nadir. We hypothesized that including both CD4 count and CD4 count minus CD4 nadir in the model would provide a more dynamic representation of the relationship between low CD4 counts and cancer risk and therefore we extended models 1 and 2 by including both CD4 count minus CD4 nadir among the parameters tested. Models were adjusted for cumulative heavy smoking (≥ 0.5 packs/day average in last 6 years of follow-up) and race; age was used as the time scale. All analyses were performed using R version 3.2.

The study population of 32 virus-associated cancer cases and 500 matched controls had a median (IQR) age and follow-up of 35 (30–42) and 21 (8–26) years, respectively (Table 1). The majority of incident cancers were anal cancers and NHL (n=9 cases each) followed by liver cancer (n=6 cases), while incident HL, HNSCC, and KS accounted for 3 cases or less (Supplemental Material 2). Virus-associated cancers comprised the first diagnosis among two of four subjects with multiple cancer diagnoses (Supplemental Material 3); in the remaining two cases, virus-associated cancers were the second primary malignancy, diagnosed 17 and 2 years after previous diagnoses of thyroid cancer and prostate cancer, respectively. Compared to controls, virus-associated cancer cases were slightly older at entry, with shorter follow-up and higher percentage with HBV infection (p≤0.003). Cases were similar to controls with regard to race, smoking, calendar period, HCV infection, number of sexual partners, and sexually transmitted infections (Table 1). Cases had a non-significant trend toward lower median CD4 cell counts compared to controls (858 vs. 947 cells/μl, respectively; p=0.15), while CD4 nadir was significantly lower (512 vs. 620 cells/μl; p=0.007) and percentage with CD4 nadir < 500 cells/μl was higher (46.9% vs. 27.4%; p=0.03). There was a trend toward lower median CD4:CD8 ratio nadir in cases compared to controls (1.62 vs. 1.85, respectively; p=0.08), while the percentage with CD4:CD8 ratio nadir < 1 was higher (56.2% vs. 29.2%; p=0.003). Median time from CD4, CD4:CD8, CD8, and WBC nadir to cancer diagnosis ranged from 7.25 to 9.75 years

Immunological parameters were first examined in exploratory analyses of individual and mean trajectories in cases and controls during follow-up, which indicated an optimal window between six and ten years prior to diagnosis for evaluation of prognostic markers based on group differences and data coverage (Supplemental Material 1 and Figures 1–3). Longitudinal trends of CD4, CD8, and WBC counts in individual virus-associated cancer cases showed variable patterns over ten years or more prior to diagnosis, including chronically low counts for all three parameters, chronically low CD4 and WBC counts only, and declining CD4 and WBC counts; representative cases with immunological lab data available over 15 years or longer are shown in Figure 1. The distribution of number of visits with immunological lab data for all cases and controls in the study cohort showed that 100%, 81.8%, and 63% of participants had immunological lab data for at least 2, 12, and 20 visits, respectively, corresponding to one, six, and ten years of follow-up (Supplemental Material 1). Given this distribution of data coverage, exploratory analyses evaluated prognostic markers over ten years for groups by cancer status and six years for groups by individual diagnoses. These exploratory analyses showed lower mean trajectories for immunological parameters, including CD4, CD8, WBC counts, and CD4:CD8 ratios, in cases compared to controls over a ten year window (Figure 2). When examined by individual diagnoses, subjects who developed NHL had slightly higher mean CD4, CD8, and WBC trajectories compared to those who developed solid-tissue tumors and controls (Figure 3).

Next, we sought to examine clinical characteristics associated with low CD4 nadir in the study cohort. Although CD4 lymphopenia is often idiopathic, previous studies showed that medical conditions associated with CD4 lymphopenia in HIV-negative individuals include cirrhosis and other advanced liver disease (16–18) Therefore, we examined liver disease-related factors in groups by CD4 nadir < 500 cells/μl (Table 2). The frequencies of HCV and HBV infection, heavy alcohol consumption, liver conditions, and cirrhosis did not differ between groups by CD4 nadir. However, HBV infection and cirrhosis were more common among cases compared to controls, regardless of CD4 nadir status. The proportion with FIB-4 scores > 1.45, a common threshold indicating liver fibrosis in HCV infection (22), was nearly twice as high in groups with CD4 count nadir < 500 cells/μl compared to those with CD4 nadir ≥ 500 cells/μl among both cases and controls (62.5% vs. 37.5%, and 34.4% vs. 20.3%, respectively). Platelet counts below the normal adult reference range (< 150 × 10⁹/L), a common finding in patients with advanced liver disease, were also more common in cases and controls with CD4 nadir < 500 cells/μl compared to corresponding groups with CD4 nadir ≥ 500 cells/μl (53.3% vs. 17.6%, p=0.001, and 32.8% vs. 17.9%, p=0.08, respectively).

Next, we sought to determine if additional immunological parameters that could influence virus-associated cancer risk were detected among subjects with low CD4 nadir. To address this question, we evaluated total T- and B-cell and white blood cell counts in groups by CD4 nadir < 500 cells/μl. Total B-cell and T-cell count nadir and median summaries were determined for each subject, and summarized by cancer diagnosis (Table 2). Total B-cell count nadir and median were lower among cases and controls with CD4 nadir < 500 cells/μl compared to those with CD4 nadir ≥ 500 cells/μl (p=0.004 and 0.02 for cases; p<0.001 and p<0.001 for controls, respectively). Trends for WBC and total T-cell counts paralleled those of CD4 cell counts; controls with CD4 nadir < 500 cells/μl had more than twice the percentage of subjects with WBC nadir < 4000 cells/μl, and nearly two-fold lower mean T-cell count nadir, compared to corresponding groups with CD4 nadir ≥ 500 cells/μl (p=0.002).

Given that prolonged antibiotic use has been linked to alterations in immune defenses (24–26), we examined self-reported duration of antibiotic use during follow-up. Antibiotic use was reported at more visits in cases and controls with CD4 nadir < 500 cells/μl compared to those with CD4 nadir ≥ 500 cells/μl among cases and controls (median 5 vs. 8 visits, p=0.003, and 3 vs. 8 visits, p=0.03, respectively). However, we did not observe a trend of antibiotic use prior to CD4 nadir.

Given differences in CD4 and WBC counts in Figures 2 and 3, we investigated the association of CD4 and WBC counts with incident virus-associated cancers within a six-year time window in mixed-effects models. An incident diagnosis of virus-associated cancer was associated with lower CD4 cell and white blood cell counts in models adjusted for age, race, heavy smoking, and FIB-4 scores > 1.45 (p=0.001 and 0.032, respectively; Figure 4 and Supplemental Material 4). High FIB-4 was independently associated with lower CD4 and white blood cell counts, while heavy smoking was associated with higher counts (Supplemental Material 4).

To examine the prognostic value of CD4 and CD8 T cell parameters relative to incident virus-associated cancers, Cox regression models were fit to CD4 cell count, CD4 cell count-nadir differential, and CD4:CD8 ratio and nadir with adjustments for age (as the time scale), race, and heavy smoking (Table 3). Lower CD4 cell count nadir showed a strong association with risk of incident virus-associated cancers (adjusted HRs/100 cells/μl decrease [95% CI]: 1.31 [1.13, 1.51]; p<0.001). Current CD4 cell count-nadir differential was a better predictor of incident virus-associated cancers (adjusted HRs/100 cells/μl decrease and 95% CI: 1.27 [1.09, 1.48], p=0.002) than recent CD4 count (adjusted HRs/100 cells/μl decrease [95% CI] 1.17 [1.03–1.33]; p=0.014). Current CD4:CD8 ratios were not associated with increased risk of virus-associated cancers (p=0.179); however, nadir CD4:CD8 ratio was associated with a 3- to 4-fold increased risk of virus-associated cancers (adjusted HRs, 0.1 unit decrease and 95% CI: 1.18 [1.06, 1.31]; p=0.002). Heavy smoking was associated with a 3- to 4- fold increased risk of virus-associated cancers, while race had no significant associations in these models (Table 3).