Leptin independently predicts development of sepsis and its outcome

Patients aged 18 years or older with a diagnosis of sepsis within 24 h after admittance to the intensive care unit (ICU) were included.

For patients with multiple admissions due to sepsis, only the first event was included. Sepsis, severe sepsis or septic shock was defined according to standard definitions [25]. Acute Physiology, Age and Chronic Health Evaluation (APACHE) II score was calculated and used for assessment of severity of illness at admission [26]. Sequential Organ Failure Assessment Score (SOFA) as a marker for organ dysfunction and disease severity was calculated at admission [27]. Data on height and weight were recorded, if present, and body mass index (BMI) was calculated as weight (kg) divided by height (m) squared. Data on length of stay, mortality, referral patterns, and reasons for admission, co-morbidities, and sources of infection, primary infection sites and causative microorganisms were collected. Microbiological cultures were considered relevant if acquired within 48 h before or after admission to the ICU. Pre-existing diseases were defined according to Knaus et al. [26].

In VIP and MONICA, participants were asked to complete a health questionnaire about their living conditions and cardiovascular risk factors, and anthropometry and blood pressure were measured. An oral glucose tolerance test with measurements of fasting and post-load glucose levels was routinely performed in VIP and in 60% of the MONICA participants but was not obtained in MSP and in NSMC. Diabetes and intermediate forms of glucose intolerance were determined according to WHO guidelines [28].

In the MONICA and MSP surveys, blood pressure was recorded in the sitting position after 5 min of rest, initially using a mercury sphygmomanometer but since 2004 by using semi-automatic devices (Omron M7, Omron Corp., Kyoto, Japan). In the VIP survey, blood pressure was measured after 5 min of rest in the recumbent position until 1 September 2009 and thereafter in the sitting position using devices as above. The measurements obtained in the recumbent position were adjusted according to a sex- and age-specific formula [29]. Hypertension was defined as systolic BP ≥140 mmHg and/or diastolic BP ≥90 mmHg and/or on anti-hypertensive medication.

Weight was measured without shoes in light indoor clothing and recorded to the nearest 0.2 kg. Height was measured to the nearest centimetre, without shoes, and BMI was calculated.

Subjects were categorized as daily smokers, ex-smokers or non-smokers. Total serum cholesterol was measured using a bench-top analyser (Reflotron^R, Boehringer Mannheim GmbH Diagnostica, Mannheim, Germany) at the time of the health survey (VIP, until 1 September 2009) or by an enzymatic method (Boehringer Mannheim GmbH Diagnostica, Mannheim, Germany) at a central laboratory (MONICA and VIP after 1 September 2009). Cholesterol values obtained using the bench-top method were adjusted to the results measured at the central laboratory.

No clinical examinations were performed in the NSMC.

Data are presented as numerical values or percentages. Non-normally distributed data were log_e-transformed prior to analysis. Continuous data are presented as (geometric) means with 95% confidence intervals (CI). Pearson correlation or Spearman’s rho was used for test of associations. For comparisons, Fisher’s exact, Student t, or Mann–Whitney U-tests were used when appropriate. Paired sample t-test was used for intra-individual comparison. Since cases and referents had the same follow-up time within strata in this nested and matched case-referent study, logistic regression analysis (rather than Cox regression) using the conditional maximum likelihood routine designed for matched analysis was uses to estimate odds ratios (OR) and 95% CIs, and the influence of studied variables on future sepsis (stratified sex) was tested in univariable and multivariable models. Missing continuous values (BMI and serum cholesterol) were replaced with the cohort- and sex-specific median values representing the referents and missing values for categorical variables were treated as a separate category (not shown in tables). Non-conditional logistic regression analysis was used to calculate the risk for in-hospital death. Leptin and adiponectin were tested both as continuous (log_e-transformed) and categorical (quartiles) variables. Cut-offs for quartiles were based on the cohort and sex-specific distribution of the baseline adipokine levels amongst referents (risk for sepsis) or amongst cases (risk for death). A p-value <0.05 was considered significant, and all p-values reported are two-sided. No adjustment was made for multiple testing. SPSS ver. 22 was used for statistical analysis.

Subject with future sepsis had marginally higher BMI and lower total cholesterol than matched referents (Table 1). Prevalences of diabetes and hypertension, fasting and post-load blood glucose levels did not differ between cases and their referents. Circulating levels of leptin and adiponectin did not differ between cases and their referents. As expected, women had higher leptin (P < 0.001) and adiponectin (P < 0.001) levels (Figs. 1 and 2, respectively).

The acute event was classified as sepsis in 26%, as severe sepsis in 52% and as septic shock in 22%, with no differences between men and women (Table 2). The ICU mortality was 18% and the hospital mortality was 21%. The median time between survey participation and event was 6.5 years (IQR 7.7). The mean age at sepsis onset was 56.1 years in women and 61.0. years in men.The frequency of co-morbidities, including diabetes, steroid treatment, and renal insufficiency at the time of the sepsis event was similar in men and women (Table 2).

At baseline, BMI correlated with high circulating levels of leptin (r = 0.36, P < 0.001), and with low circulating levels of adiponectin (r = −0.24, P < 0.001). In contrast, BMI did not associate with leptin (r = −0.05, P = 0.60) or with adiponectin (r = −0.05, P = 0.44) in the acute phase. Furthermore, leptin and adiponectin levels in the acute phase did not correlate with severity of disease expressed as APACHE- (leptin; P = 0.95, adiponectin; P = 0.79) or SOFA- scores (leptin; P = 0.88, adiponectin; P = 0.94). Leptin and adiponectin did not correlate at baseline (P = 0.14) or in the acute phase (P = 0.92).

High circulating levels of leptin predicted a first-ever sepsis event (OR 2.04, 95% CI 1.30–3.2, P = 0.002) and retained predictive value after adjustment for BMI (OR 1.89, 95% CI 1.14–3.13, P = 0.01) and in the fully adjusted model (OR 1.77, 95% CI 1.04–3.00, P = 0.03) (Fig. 2). None of the included confounders remained significantly associated with sepsis in the fully adjusted model (data not shown). The septic event was graded as sepsis, severe sepsis or septic shock, and a graded response was seen in that there were stronger BMI-independent associations between hyperleptinemia and more severe forms of sepsis compared to milder forms of sepsis. Furthermore, leptin predicted sepsis-related in-hospital deaths (Fig. 2). Stratified for sex hyperleptinemia predicted sepsis in both men (OR 2.39, 95% CI 1.18–4.86, P = 0.02) and women (OR 1.83, 95% CI 1.02–3.27, P = 0.04). This association remained in men after adjustment for BMI (OR 2.60, 95% CI 1.20–5.61, P = 0.02), but not in women (P = 0.36). Furthermore, leptin predicted independently in-hospital death in men (OR 6.41 95% (1.32–31.1, P = 0.02). Adiponectin levels were not associated with the development of sepsis in any model (data not shown).

Contrary to baseline, there were no differences in leptin- or adiponectin levels between men and women in the acute phase (leptin; P = 0.26, adiponectin; P = 0.36), (Fig. 3). However, the increase in both leptin- and adiponectin levels between baseline and the acute phase were significantly higher in men than in women (leptin P = 0.001, adiponectin P = 0.02). Leptin levels increased from baseline to the acute phase in surviving men (P = 0.001) whereas surviving women decreased their leptin levels from baseline to the acute phase (P = 0.02) (Fig. 4a). There was no significant change in leptin levels from baseline to the acute phase in non-survivors (men; P = 0.09, women; P = 0.31) (Fig. 4a).

Adiponectin levels increased from baseline to the acute phase in both surviving and non-surviving men whereas surviving and non-surviving women decreased their adiponectin levels from baseline to the acute phase, however the changes were not statistically significant (Fig. 4b).

High leptin levels expressed as the highest three quartiles compared to the lowest quartile predicted death irrespective of disease severity (APACHE II or SOFA score) in women (OR 4.18, 95% CI 1.17–15.00, P = 0.03), whereas high leptin levels in men were associated with a decreased risk of death (OR 0.05, 95% CI 0.01–0.48, P = 0.01) (Fig. 5). Adjustment with SOFA score gave similar point estimates. Furthermore, leptin levels were dichotomised using a single cut-off for both men and women (10 ng/mL). Levels above 10 ng/mL were significantly associated with in hospital death, OR 2.48, 95% (1.06–5.77, P = 0.035), which remained after adjustment for APACHE II; OR 2.68, 95% CI (1.08–6.65), P = 0.033, but not after adjustment for SOFA score, OR 2.15 95% CI (0.86–5.39), P = 0.10.

This risk for in-hospital death remained in women, OR 7.48, 95% CI (2.30–24.28), P = 0.001, but not in men, OR 0.49, 95% CI (0.12–1.95), P = 0.31. When analyzed as a continuous log_e-transformed variable, high leptin in the acute phase predicted in-hospital death independently of APACHE II-score in women (OR 1.58, 95% CI 1.01–2.48, P = 0.04), whereas the protective effect of high leptin levels in men did not remain significant (OR 0.80, 95% CI 0.42–1.49, P = 0.48).

Adiponectin did not associate with in-hospital death, neither as a categorical variable, nor as a continuous variable (Fig. 5).