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What’s new? Accurate diagnosis of cardiac implantable electronic device infections and especially pocket infections is of paramount importance to avoid delayed removal of infected systems and unnecessary extraction of non-infected systems. Our study prospectively validates the diagnostic utility of procalcitonin (PCT) with a cut-off value of 0.05 ng/ml for the diagnosis of a pocket infection and supports its value in comparison to classic inflammatory markers. PCT could also be useful for patients who are difficult to diagnose clinically, such as patients pre-treated with antibiotics or with minimal local inflammatory signs. Low PCT values may assist in ruling out pocket infection and avoiding unnecessary surgical pocket exploration. |
Introduction
Cardiac implantable electronic devices (CIEDs) such as pacemakers, implantable cardiac defibrillators (ICDs), and cardiac resynchronization therapy (CRT) devices are essential for the treatment of bradyarrhythmias and important elements of optimal, guideline-directed treatment of heart failure and life-threatening tachyarrhythmias [1]. One of the main complications of CIEDs are cardiac device infections (CDI), which are associated with increased morbidity and mortality, as well as increased healthcare costs [1, 2].
With the increasing number of CIED implants [1], the incidence of CDI is also rising, but unfortunately at a disproportionate rate [3, 4]. The increase in CDI rates has been attributed to the use of more complex devices in a more comorbid and elderly population, in which the risk of infection is intrinsically higher [1, 3, 4]. Preventive measures include perioperative antibiotic therapy and implantation of local antimicrobial agents or a combination of both strategies [5].
To identify patients at risk for CDI in a clinical setting, several risk scores have been proposed [1, 6]; however, over 60 studies and several meta-analyses aimed to identify potential risk factors for CDI have yielded inconsistent results [7]. Recently the PADIT (Prevention of Arrhythmia Device Infection Trial) score has been developed from a retrospective analysis of over 19 000 patients (from the PADIT trial) [8]. The PADIT score classifies patients at low, intermediate, or high risk of CDI based on 5 independent predictors of device infection: age, renal function, immune deficiency, number, and type of prior CEID procedures [2].
An international consensus document on the risk assessment, prevention, diagnosis, and treatment of CDI has been published to support the diagnosis and management of CDIs [1]. Depending on the extent and severity of the infection, three categories of CDI are distinguished: (1) pocket infections; (2) CIED systemic infections; (3) lead-related infective endocarditis [1]. While CIED systemic infections and lead-related infective endocarditis are associated with bacteremia and systemic inflammatory response, pocket infections are limited to the generator pocket [1, 9]. As such, their diagnosis to date relies on clinical judgment based on local inflammation signs, such as erythema, warmth, swelling, tenderness, or, in severe cases, purulent drainage [1, 9].
Given the heterogeneous presentation of patients with pocket infections, often with few or mild symptoms, the diagnosis is often challenging and can be missed in the early stages. However, early diagnosis and aggressive treatment of pocket infections are vital to avoid progression to systemic infection, infective endocarditis, and sepsis [1]. A pocket infection is a class I indication for complete device system removal [1], and conservative antimicrobial treatment without immediate device removal was associated with a 7-fold increase in 30-day and 3-fold increase in 1-year mortality in multivariate analysis [10]. On the other hand, non-invasive exclusion of pocket infection avoids unnecessary surgical pocket explorations and complications related to device removal [1, 10].
Identification of relevant biomarkers to aid diagnosis of such pocket infection is thus of vital importance. Conventional systemic inflammation parameters, such as leukocytosis, elevated C-reactive protein (CRP) levels, or erythrocyte sedimentation rate, can be indicative of systemic CDIs, but are non-specific and often within the normal range in pocket infection [11, 12]. An exploratory biomarker study in confirmed pocket infection cases identified procalcitonin (PCT) as a marker of pocket infection out of 14 different biomarkers including white blood cell count (WBC) and CRP. With receiver operating characteristic (ROC) analysis and Youden statistic, an optimized cut-off value of 0.05 ng/ml PCT was identified, 10-fold lower than the established cut-off value of 0.5 ng/ml used clinically for diagnosing sepsis. Using this optimized cut-off value of 0.05 ng/ml, PCT could predict the presence of pocket infection with a sensitivity of 60% and specificity of 82% [12].
This study aims to prospectively validate the PCT cut-off value of 0.05 ng/ml as a biomarker of pocket infection and to assess its sensitivity and specificity in distinguishing pocket infections from infection-free controls. In a secondary analysis, we compare inflammatory markers including PCT between patients with pocket infection and systemic CDI.
Methods
The trial is designed as a case-control validation study based on a prospective single-center register of a cohort of CIED recipients with and without CIED infection. The study was approved by the local ethic committee and conducted according to the principles of the Declaration of Helsinki. The study was registered at ClinicalTrials.gov with the identifier NCT05007158.
Study population
All patients with confirmed isolated pocket infection, CIED systemic infection, or lead-related infective endocarditis treated at the German Heart Center Munich between December 2011 and May 2021 were included. Patients presenting for elective device exchange or planned lead revision without local or systemic infections were selected as controls. Patients with concomitant infectious or inflammatory diseases, recent trauma, surgery, or burns, as well as patients with current active malignancy or receiving immunosuppressive therapy, were excluded. Patients with end-stage renal failure (defined as glomerular filtration rate ≤25 ml/min or on renal dialysis) were also excluded. The study group and the control group were matched for age and renal function.
All patients were evaluated for the presence of isolated pocket infections, CIED systemic infections, and lead-related infective endocarditis. Lead-associated infective endocarditis was diagnosed according to the modified Duke criteria [13]. CIED systemic infections were diagnosed as the presence of pocket infection accompanied by bacteremia or echocardiographic finding suggestive of infective endocarditis, but not fulfilling the Duke criteria. Isolated pocket infection was diagnosed in the presence of local signs of inflammation (one or more of erythema, pain, warmth, swelling, induration, tenderness, or fluctuation), wound dehiscence, hardware protrusion, or pus discharge at the pocket in the absence of systemic findings. The diagnosis was confirmed by surgical exploration of the generator pocket site.
All patients were treated according to clinical guidelines with a transvenous removal of all hardware material. All patients underwent laboratory workup including PCT, CRP, WBC, and peripheral blood cultures at admission before surgery. Microbiological cultures of intraoperative smears, biopsies of pocket tissue, and extracted lead tips were obtained for patients with local pocket infection, systemic CIED infection, and lead-associated infective endocarditis.
Outcomes
For our primary analysis, we assessed the diagnostic value of PCT in differentiating local pocket infection from infection-free controls and calculated the sensitivity and specificity of the pre-established cut-off value of 0.05 ng/ml. As pre-specified subgroup analyses, we calculated sensitivity and specificity of PCT with a cut-off value of 0.05 ng/ml in patients with and without antibiotic pretreatment, as well as in patients with minimal or extensive local inflammation. Any antibiotic administration before admission was considered antibiotic pretreatment, irrespective of type or duration of therapy. For the subgroup analysis of minimal or extensive local inflammation, all patients with signs of wound dehiscence or hardware protrusion were excluded, as skin perforation itself is diagnostic for pocket infection [1]. The remaining patients were classified according to the number of local inflammatory signs having a “minimal local inflammation” with up to two local inflammation signs or having “extensive local inflammation” with more than two out of the following signs: erythema, pain, warmth, swelling, induration, tenderness, or fluctuation.
We assessed sensitivity and specificity of the conventional inflammatory markers CRP and WBC with the respective, clinically established, cut-off values of 5 mg/dl and 109/l. Finally, we compared the values of all inflammatory markers between local pocket infections and systemic CIED infections, and lead-associated infective endocarditis.
Statistical analysis
All statistical analyses were performed using SPSS V22 (IBM Corporation, Armonk, NY, US). Categorical data are presented as absolute and relative frequencies and continuous data as median with interquartile range (IQR). The diagnostic accuracy of PCT with the pre-established cut-off value of 0.05 ng/ml was described by values of sensitivity and specificity. ROC curves were drawn and the area under the ROC curve (AUC) with 95% confidence intervals (95% CI) was calculated. Comparisons were performed using either the Pearson χ2 or the Fisher exact tests for categorical variables as appropriate. Continuous variables were analyzed using the Mann-Whitney U test or the Kruskal-Wallis test as appropriate. We considered a P-value <0.05 to result in statistically significant differences.
Results
Baseline characteristics
Between 2011 and April 2021, 81 patients with pocket infection, 23 patients with CIED systemic infection, and 34 with lead-related infective endocarditis were identified. Another 81 patients matched for age and renal function and presenting for device exchange or lead revision unrelated to infection were included as controls.
Baseline characteristics are shown in Tables 1 and 2. There was no significant difference in age, sex, presence of diabetes, kidney failure, or device type between the pocket infection group and the control group. The median interval from the previous CIED procedure was shorter in the pocket infection group (0.7 [IQR, 0.1–2.3] years vs. 7.8 [IQR, 3.9–9.6] years; P <0.001), as well as the median implant duration (7.4 [IQR, 2.2–13.1] years vs. 9.6 [IQR, 7.2–12.5] years; P = 0.03).
|
Characteristic |
Pocket infection (n = 81) |
Control group (n = 81) |
P-value |
|
Age, years |
77.0 (67.8–82.5) |
73.2 (63.9–80.1) |
0.074 |
|
Male sex |
60 (74) |
64 (79) |
0.458 |
|
Diabetes mellitus |
21 (26) |
27 (33) |
0.302 |
|
Device at presentation |
|
|
0.882 |
|
Device, DDD-PM |
40 (49) |
39 (48) |
|
|
Device, VVI-PM |
2 (3) |
3 (4) |
|
|
Device, DDD-ICD |
8 (10) |
7 (9) |
|
|
Device, VVI-ICD |
10 (12) |
15 (19) |
|
|
Device, CRT-D |
18 (22) |
15 (19) |
|
|
Device, CRT-P |
3 (4) |
2 (3) |
|
|
Number of leads |
2.0 (2.0–3.0) |
2.0 (2.0–2.0) |
0.004 |
|
Years since first CIED implantation |
7.4 (2.2–13.1) |
9.6 (7.2–12.5) |
0.030 |
|
Years since last CIED procedure |
0.7 (0.1–2.3) |
7.8 (3.9–9.6) |
<0.001 |
|
PADIT score |
8.5 (4.0–9.0) |
4.0 (2.0–9.0) |
0.004 |
|
Creatinine, mg/dl |
1.07 (0.94–1.35) |
1.07 (0.92–1.35) |
0.856 |
|
GFR, ml/min/1.73 m2 |
65 (50–83) |
70 (53–84) |
0.351 |
|
Characteristic |
Pocket infection |
CIED systemic infection |
Lead-related infective endocarditis |
P-value |
|
Number, n |
81 |
23 |
34 |
|
|
Age, years |
77.0 (67.8–82.5) |
72.0 (62.7–80.8) |
73.4 (66.2–78.5) |
0.187 |
|
Sex, male |
60 (74) |
19 (83) |
26 (77) |
0.697 |
|
Diabetes mellitus |
21 (26) |
6 (26) |
14 (41) |
0.242 |
|
Device at presentation |
|
|
|
0.232 |
|
Device, DDD-PM |
40 (49) |
9 (39) |
8 (24) |
|
|
Device, VVI-PM |
2 (3) |
0 (0) |
0 (0) |
|
|
Device, DDD-ICD |
8 (10) |
3 (13) |
3 (9) |
|
|
Device, VVI-ICD |
10 (12) |
4 (17) |
7 (20) |
|
|
Device, CRT-D |
18 (22) |
7 (30) |
12 (35) |
|
|
Device, CRT-P |
3 (4) |
0 (0) |
4 (12) |
|
|
Number of leads |
2.0 (2.0–3.0) |
2.0 (2.0–3.0) |
2.0 (2.0–3.0) |
0.835 |
|
Years since first CIED implantation |
7.4 (2.2–13.1) |
6.3 (1.2–15.9) |
4.0 (1.9–7.9) |
0.094 |
|
Years since last CIED procedure |
0.7 (0.1–2.3) |
0.8 (0.2–3.1) |
2.3 (0.6–4.2) |
0.133 |
|
PADIT score |
8.5 (4.0–9.0) |
5.0 (4.0–9.0) |
5.0 (3.0–9.0) |
0.152 |
|
Creatinine, mg/dl |
1.07 (0.94–1.35) |
1.08 (0.93–1.65) |
1.29 (0.94–1.78) |
0.109 |
|
GFR, ml/min/1.73 m2 |
65 (50–83) |
52 (41–73) |
44 (34–76) |
0.021 |
Patients with pocket infections had significantly higher PADIT scores than infection-free controls, despite similar age, renal function, and CIED device type at presentation (median, 8.5 [IQR, 4.0–9.0] vs. 4.0 [IQR, 2.0–9.0]; P = 0.004). This difference was also noted when analyzing the CDI group as a whole, including pocket infections, CIED systemic infections, and lead-associated infective endocarditis (6.0 [IQR, 4.9–9.0] for CDI vs. 4.0 [IQR, 2.0–9.0] for controls; P = 0.014). Overall, 36% (48/134) of patients with CDI were at low, 19% (26/134) at intermediate, and 45% (60/134) at high risk for infection, whereas in the infection-free control group 52% (42/81), 12% (10/81), 36% (29/81) of patients were at low, intermediate, and high risk for infection, respectively (Figure 1).
Microbiological results
A pathogen was identified in 82% (66/81) of the pocket infection group. Out of patients with a pocket infection, 76% (60/79) had a positive culture from an intraoperative smear, 63% (50/79) from extracted lead tips, and 60% (40/67) from a tissue biopsy of the infected pocket. Patients with lead-associated infective endocarditis had positive blood cultures in 88% (30/34) of cases, positive lead tip cultures in 42% (14/33), positive intraoperative smears in 19% (6/31), and positive tissue biopsy culture in only 7% of cases (1/14). Patients with CIED systemic infections had high rates of positive cultures from intraoperative smears (86%, 18/21) and tissue biopsies (85%, 17/20) similar to pocket infections, but they had higher rates of positive blood cultures (52%, 12/23) and culture-positive lead tips (77%, 17/22).
The results of the microbiological cultures are shown in Supplementary material, Table S1. The most commonly identified bacteria in pocket infection were coagulase-negative staphylococci. Most systemic CIED infections had a similar bacterial spectrum as pocket infections, whereas staphylococcus aureus was the predominant pathogen in lead-associated infective endocarditis and some systemic CIED infections.
Antibiotic pretreatment was frequent in patients with lead-associated infective endocarditis (91%, 31/34), but also present in about one-third of patients with systemic CIED infections (39%, 9/23) and with isolated pocket infection (32%, 26/81). Patients with pocket infections pre-treated with antibiotics received antibiotics for a median (IQR) of 3 (2.0–6.3) days. Cefuroxime was most commonly prescribed (31%, 8/26), followed by Ampicillin/Sulbactam (14%, 4/26), Ceftriaxone (8%, 3/26), or Piperacillin/Tazobactam (8%, 3/26).
Biomarkers for diagnosing a pocket infection
Median values of the biomarkers PCT, CRP, and leukocytes are shown in Table 3.
|
|
Pocket infection |
CIED systemic infection |
Lead-related infective endocarditis |
Control group |
P-value |
|
PCT, ng/ml |
0.06 (0.05–0.09) |
0.08 (0.55–0.43) |
0.28 (0.12–1.39) |
0.04 (0.03–0.05) |
<0.001 |
|
CRP, mg/dl |
5.1 (1.7–12.0) |
14.0 (4.2–55.4) |
68.1 (31.8–124.0) |
1.4 (0.7–2.6) |
<0.001 |
|
Leukocytes, 109/l |
7.1 (6.2–8.9) |
8.3 (7.2–9.7) |
8.6 (6.3–11.4) |
6.7 (5.5–8.0) |
<0.001 |
The PCT level was significantly elevated in all 3 sub-types of CIED infection compared to the control group (Figure 2).
Prognostic value of PCT cut-off value 0.05 ng/ml
An elevated PCT over 0.05 ng/ml was found in 68% (55/81) of pocket infections, 78% (18/23) of CIED systemic infections, 88% (30/34) of lead-associated infective endocarditis, and 24% (19/81) of controls. Using the pre-defined cut-off value of 0.05 ng/ml, PCT had a sensitivity of 75% and a specificity of 77% for diagnosing any CDI (pocket infections, CIED systemic infections and lead-associated infective endocarditis, positive predictive value [PPV] 84%, negative predictive value [NPV] 64%; P <0.001). In ROC analysis, PCT showed an AUC of 0.81 (95% CI, 0.76–0.87; P <0.001) for differentiating CDI from controls (Figure 3A).
The sensitivity and specificity for PCT dichotomized at 0.05 ng/ml PCT for discrimination of isolated pocket infections from controls were 68% and 77%, respectively (P <0.001, Table 4).
|
PCT, 0.05 ng/ml |
N |
Sensitivity, % |
Specificity, % |
PPV, % |
NPV, % |
P-value χ²-test |
AUC (95% CI) |
P-value ROC |
|
All pocket infections |
81 |
68 |
77 |
74 |
71 |
<0.001 |
0.75 (0.676–0.829) |
P <0.001 |
|
Subgroup analyses |
|
|||||||
|
Pocket infections with antibiotic-pretreatment |
26 |
65 |
77 |
47 |
87 |
<0.001 |
0.70 (0.57–0.84) |
P = 0.002 |
|
Pocket infections without antibiotic-pretreatment |
55 |
69 |
77 |
67 |
79 |
<0.001 |
0.78 (0.69–0.86) |
P <0.001 |
|
Pocket infections with extensive local findings |
40 |
70 |
77 |
60 |
84 |
<0.001 |
0.77 (0.68–0.86) |
P <0.001 |
|
Pocket infections with minimal local findings |
9 |
67 |
77 |
24 |
95 |
0.012 |
0.75 (0.54–0.96) |
P = 0.014 |
The ROC analyses revealed an AUC of 0.75 (95% CI, 0.68–0.83; P <0.001, Figure 3B and Table 4). Thus, the results are in line with those of the former DIRT study (Figure 4).
To further assess the diagnostic value of PCT with a cut-off of 0.05 ng/ml for identifying local pocket infections, a subgroup analysis of patients pre-treated with antibiotics and patients with minimal local signs of inflammation was performed. The results are summarized in Table 4 and Figure 3C–F. Analyzing only treatment-naïve patients, PCT with a cut-off value of 0.05 ng/ml had a sensitivity of 69% for detecting local pocket infections, whereas it fell to 65% in patients with antibiotic pretreatment. Comparing patients with extensive and minimal signs of inflammation, the cut-off value of 0.05 ng/ml PCT yielded a specificity of 70% and 67%, respectively. Similarly, the ROC analyses for PCT showed an AUC of 0.78 (95% CI, 0.69–0.86; P <0.001) and 0.70 (95% CI, 0.57–0.84; P = 0.002) for patients with without and with antibiotic pretreatment, as well as 0.77 (95% CI, 0.68–0.86; P <0.001) and 0.75 (95% CI, 0.54–0.96; P = 0.014) for patients with pronounced or discrete local inflammation signs, respectively.
Conventional biomarkers (leukocytosis and CRP)
Leukocytosis, defined as leukocyte levels count above 109/l according to routine clinical cut-off values, had a similar incidence in pocket infection and controls (12% vs. 4% respectively; P = 0.079). Leukocytosis was more common in patients suffering from CIED systemic infections and lead-associated infective endocarditis, affecting 22% (5/23) and 35% (12/34), respectively. The sensitivity of leukocytosis for diagnosing a local pocket infection was 12%, the specificity 96% (PPV, 77%; NPV, 52%; P = 0.079).
An elevated CRP concentration over 5 mg/dl was found in 14% of controls, 49% of pocket infections, 61% of CIED systemic infections, and 100% of lead-associated infective endocarditis (P <0.001). The sensitivity of CRP with a cut-off of 5 mg/dl for diagnosing a local pocket infection was 49%, the specificity 86% (PPV, 78%; NPV, 63%; P <0.001).
Discussion
In the present study, we aimed to prospectively validate the diagnostic value of PCT with an optimized cut-off of 0.05 ng/ml for diagnosing CIED pocket infections in a real-world setting. This optimized cut-off value is 10-fold lower than the established cut-off used for diagnosing sepsis. We found that PCT with the cut-off of 0.05 ng/ml had a sensitivity of 68%, a specificity of 77%, PPV of 74%, and an NPV of 71% for detecting a local pocket infection. These results are in line with the exploratory study that identified PCT as a promising biomarker to diagnose local pocket infection, which found a sensitivity of 60% and a specificity of 82% for PCT with a cut-off of 0.05 ng/ml (Figure 4) [12].
Age and renal impairment can influence inflammation and therefore PCT levels; this potential bias was minimized by matching the control group for these two variables. Renal impairment affects PCT levels only mildly [14], and PCT has been proven to accurately diagnose infections in patients with kidney disease [15].
To further analyze the diagnostic value of PCT for diagnosing local pocket infection in a real-world setting, we analyzed the influence of antibiotic pretreatment on its sensitivity and specificity. PCT levels respond rapidly to antibiotic treatment [16] and a lack of decrease during antibiotic treatment is associated with an increase in in-hospital mortality in sepsis patients [17]. Consistently, in our study, the sensitivity of a positive PCT result increased to 69% if only patients without antibiotic pretreatment were analyzed, whilst it fell to 65% in patients pre-treated with antibiotics. The relatively small change in sensitivity despite antibiotic pretreatment with a mean duration of 3 days suggests PCT values above 0.05 ng/ml remain a robust marker for pocket infections even in patients already treated with antibiotics.
Besides pretreatment, a subtle or atypical clinical presentation makes diagnosing pocket infections even more difficult. Diagnosing a pocket infection is straightforward where extensive local inflammatory, wound dehiscence, hardware protrusion, or pus discharge at the pocket are present [1, 9]. In more subtle cases with minimal local inflammation signs, the diagnosis can be easily missed [9]. A clinically unremarkable pocket infection with few or no inflammation signs is challenging to diagnose even for an experienced clinician, demanding auxiliary diagnostic tools, such as biomarkers [9]. However, the extent of local inflammation might also influence PCT values [18], and as such the sensitivity of a positive PCT value would be expected to be lower. Though we did see a lower sensitivity of PCT in patients with minimal inflammatory signs (67% vs. 70%), the difference was relatively small and unlikely to be of clinical relevance. Furthermore, the sensitivity of PCT remained significantly higher than that of CRP or leukocytosis (49% and 12% respectively). Importantly, the high NPV of 95% for PCT even in patients with minimal local inflammatory signs might help to identify patients without pocket infections and thus prevent unnecessary pocket explorations or device extractions.
Although CRP was better than leukocytosis, both have limited use in diagnosing pocket infections, especially considering the already pre-selected patient cohort. Patients with isolated pocket infections do not present with leukocytosis; median leukocyte counts were not elevated with 7.1 (IQR, 6.2–8.9) 109/l. Thus, white blood count yields only little diagnostic value and the absence of leukocytosis does not exclude a local pocket infection, as previously shown [12, 19–21]. CRP is synthesized in response to infections, both bacterial and viral, but also to other causes of systemic inflammation, such as trauma or autoimmune diseases [22]. As our study excluded patients with conditions that might influence inflammation parameters, such as active malignancies, recent operations, or burns, the specificity of CRP might be even lower in a real-life clinical setting. On the contrary, PCT seems to be a more accurate biomarker for identifying infections and is known to differentiate bacterial from viral causes [16, 22]. Thus, PCT seems more helpful than conventional biomarkers for diagnosing pocket infection even in challenging clinical situations, such as antibiotic pretreatment or subtle clinical presentation.
In our study, PCT levels were significantly higher in patients with systemic CIED infections and lead-associated infective endocarditis compared to pocket infections (Table 3). As PCT levels indicate the extent of systemic manifestation and disease severity [18, 23], exceptionally high PCT levels may help to identify patients suffering from systemic CIED infection or even lead-related infective endocarditis and have subsequent influences on antibiotic treatment duration.
Besides validating PCT as a diagnostic biomarker for pocket infections, our study also supports the moderate predictive power of the PADIT score [2] for CIED infections. In our cohort, patients suffering from pocket infection or any CIED infections had significantly higher PADIT scores than infection-free controls, despite similar age, renal function, and CIED devices at presentation lending credence to the predictive nature of the number of prior CIED interventions which explains the difference in the PADIT scores in our cohorts. Although there were no differences between the pocket infection and control groups regarding the type of device, those with pocket infections had a greater number of leads. That finding was consistent with the PADIT study results, according to which CRT poses a higher infection risk than non-CRT devices. Nevertheless, 36% of the infection-free control group were considered at high risk for infection by the PADIT score. Thus, the control group appears adequately balanced in regard to the risk of CDI.
The microbiological spectrum with a predominance of staphylococcus species detected in our study is consistent with previous reports [24, 25]. The microbiological spectrum differed between the subgroups of CDIs, with coagulase-negative staphylococci being the main pathogen in the local pocket infections, as well as systemic CDIs and staphylococcus aureus in lead-associated infective endocarditis, as previously shown [25]. This finding supports different pathogenesis behind pocket infections, primarily transdermal infections, and lead-associated infective endocarditis, hematological seeding due to bloodstream infection, as well as migration from an infected pocket to the leads.
Strengths and limitations
The main strength of our study is the prospective design in a real-world clinical setting and the large cohort. Given the high rates of positive microbiological cultures in our patients with pocket infections, our cohort has high internal validity.
A possible limitation of our study is that patient numbers in the sub-group analyses are relatively small and so these results should be interpreted with caution. Given that sub-groups such as antibiotic pre-treated patients are a rare entity, this study represents the largest cohort in the literature on the subject. We also excluded patients with active malignancies or burns, with recent operations or traumata, on immunosuppression and end-stage renal failure. Therefore, the diagnostic relevance of PCT in these special patient populations would require further research.
Conclusion
Our study validates the diagnostic utility of a cut-off value of 0.05 ng/ml PCT for the diagnosis of a pocket infection. The diagnostic value of 0.05 ng/ml PCT may be clinically useful for patients who are difficult to diagnose clinically, such as patients pre-treated with antibiotics or with minimal local inflammatory signs. Furthermore, PCT levels were significantly higher in patients with systemic CIED infections and lead-associated infective endocarditis, which differentiates them from local pocket infections.
Supplementary material
Supplementary material is available at https://journals.viamedica.pl/kardiologia_polska.
Article information
Conflict of interest: None declared.
Funding: None.
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