A nested case-control study of 277 prediagnostic serum cytokines and glioma

Schwartzbaum, Judith A.; Wang, Min; Root, Elisabeth Dowling; Pietrzak, Maciej; Rempała, Grzegorz A.; Huang, Rong‐Yau; Johannesen, Tom Børge; Grimsrud, Tom Kristian

doi:10.1371/journal.pone.0178705

Cited by 16 publications

(38 citation statements)

References 41 publications

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“…Only one other study of glioma, conducted in Norway (JSBC study), assessed pre-diagnostic cytokine levels. 23,24 While the current and JSBC study are similar in size (457 and 487 case/control sets, respectively), the JSBC investigators used a single pre-diagnostic serum sample to measure 277 cytokines. 23,24 They found five cytokines (VEGF, beta-Catenin, CCL22, LIF, and sIL10RB) to be significantly associated with risk of glioma at different time periods prior to glioma diagnosis, i.e., discovery rate within the false positive range; the associations with IL-15 and IL-16 in that study were null.…”

Section: Discussionmentioning

confidence: 99%

“…20–22 Also, a recent case-control study nested in the Janus Serum Bank Cohort (JSBC) in Norway assessed 277 cytokines and identified five (sIL10RB, VEGF, beta-Catenin, CCL22, and LIF) independently related to glioma risk in one of five periods prior to glioma diagnosis based on a single pre-diagnostic sample. 23,24 These findings remain unconfirmed.…”

Section: Introductionmentioning

confidence: 98%

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Serially measured pre-diagnostic levels of serum cytokines and risk of brain cancer in active component military personnel

et al. 2018

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Background There is growing evidence that history of allergic or autoimmune disease is associated with reduced risk of glioma, but few prospective studies have explored the biological basis. To assess associations with immune conditions and levels of 14 cytokines in serial prediagnostic serum samples, we conducted a study of glioma/brain cancer nested in a cohort of active component military personnel. Methods A total of 457 case-control sets were ascertained from the Department of Defense (DoD) Automated Central Tumour Registry, Defense Medical Surveillance System (DMSS) database, and DoD Serum Repository. These were individually matched on sex, race/ethnicity, birth year, number of serum samples (1, 2 or 3), and date(s) of sample collection. We obtained diagnoses of pre-existing immune-related conditions from the DMSS database and measured cytokines using Meso Scale Discovery assays. Statistical analyses included conditional logistic regression. Results Overall association between glioma and prior immune-related conditions was null. Higher levels of IL-15 and IL-16 were independently associated with lower glioma risks ( P trend = 0.002 and P trend = 0.001); both associations were more pronounced in individuals with prior immune conditions ( P heterogeneity = 0.0009 and P heterogeneity = 0.031). Conclusions Associations with pre-diagnostic levels of IL-15 and IL-16 and their modification by diagnosis of immune-related conditions support the importance of immune alterations in glioma aetiology years before diagnosis.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 98%

Serially measured pre-diagnostic levels of serum cytokines and risk of brain cancer in active component military personnel

et al. 2018

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“…follow the same multivariate distribution). This can already be a problem if the number of variables (cytokines) is only ~10 13 , and is greatly exacerbated if the number of variables grows large, which is the case for current research where even hundreds 14 of cytokines are analysed simultaneously. The problem of anomaly detection for many-variable data sets is even worse in the case of ratios: For d variables, there are ratios which grows large very quickly, even for modest d .…”

Section: High-dimensional Datamentioning

confidence: 99%

Establishing a many-cytokine signature via multivariate anomaly detection

Dingle

Zimek

Azizieh

et al. 2019

Sci Rep

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Establishing a cytokine signature associated to some medical condition is an important task in immunology. Increasingly, large numbers of cytokines are used for signatures, via lists of reference ranges for each individual cytokine or ratios of cytokines. Here we argue that this common approach has weaknesses, especially when many different cytokines are analysed. Instead, we propose that establishing signatures can be framed as a multivariate anomaly detection problem, and hence exploit the many statistical methods available for this. In this framework, whether or not a given subject’s profile matches the cytokine signature of some condition is determined by whether or not the profile is typical of reference samples of that condition, as judged by an anomaly detection algorithm. We examine previously published cytokine data sets associated to pregnancy complications, brain tumours, and rheumatoid arthritis, as well as normal healthy control samples, and test the performance of a range of anomaly detection algorithms on these data, identifying the best performing methods. Finally, we suggest that this anomaly detection approach could be adopted more widely for general multi-biomarker signatures.

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“…In an attempt to better understand the link between immunity and brain cancer, Schwartzbaum went back to the archived Norway blood samples and measured the levels of various immune-system proteins called cytokines in people with glioma, years before their diagnosis 6 . She expected to find that people who went on to develop glioma had lower levels of cytokine than did those who did not develop the cancer.…”

Section: Nothing To Sneeze Atmentioning

confidence: 99%

Searching for the roots of brain cancer

Savage

2018

Nature

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A nested case-control study of 277 prediagnostic serum cytokines and glioma

Cited by 16 publications

References 41 publications

Serially measured pre-diagnostic levels of serum cytokines and risk of brain cancer in active component military personnel

Serially measured pre-diagnostic levels of serum cytokines and risk of brain cancer in active component military personnel

Establishing a many-cytokine signature via multivariate anomaly detection

Searching for the roots of brain cancer

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