Abstract
Purpose
Patients with fever and inflammation of unknown origin (FUO/IUO) are clinically challenging due to variable clinical presentations with nonspecific symptoms and many differential diagnoses. Positron emission tomography/computed tomography (PET/CT) with 2-deoxy-2-[18F]fluoro-D-glucose ([18F]FDG) is increasingly used in FUO and IUO, but the optimal diagnostic strategy remains controversial. This consensus document aims to assist clinicians and nuclear medicine specialists in the appropriate use of [18F]FDG-PET/CT in FUO and IUO based on current evidence.
Methods
A working group created by the EANM infection and inflammation committee performed a systematic literature search based on PICOs with “patients with FUO/IUO” as population, “[18F]FDG-PET/CT” as intervention, and several outcomes including pre-scan characteristics, scan protocol, diagnostic yield, impact on management, prognosis, and cost-effectiveness.
Results
We included 68 articles published from 2001 to 2023: 9 systematic reviews, 49 original papers on general adult populations, and 10 original papers on specific populations. All papers were analysed and included in the evidence-based recommendations.
Conclusion
FUO and IUO remains a clinical challenge and [18F]FDG PET/CT has a definite role in the diagnostic pathway with an overall diagnostic yield or helpfulness in 50–60% of patients. A positive scan is often contributory by directly guiding treatment or subsequent diagnostic procedure. However, a negative scan may be equally important by excluding focal disease and predicting a favorable prognosis. Similar results are obtained in specific populations such as ICU-patients, children and HIV-patients.
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Introduction
Imaging of infection and inflammation has been part of nuclear medicine since the 1970s with the use of [67Ga]Ga-citrate, radiolabelled white blood cells, and finally the glucose analog 2-deoxy-2-[18F]-fluoro-D-glucose ([18F]FDG). In the first decade of [18F]FDG PET, incidental [18F]FDG uptake in infectious or inflammatory foci in cancer patients was considered a false-positive nuisance, but from the 1990s onward, this changed with a greater understanding and appreciation of [18F]FDG PET in infectious and inflammatory conditions [1, 2].
An early application of [18F]FDG PET in infectious and inflammatory diseases was fever of unknown origin (FUO), a heterogeneous and clinically challenging condition with a multitude of underlying differential diagnoses, i.e. infections, non-infectious inflammatory diseases (NIID), malignancies, and miscellaneous [3,4,5,6,7,8,9]. The definition of FUO has changed several times since the original definition from 1961 [10]; the current definition includes fever > 38.3° C on more than three occasions during more than three weeks with no clear diagnosis despite three days of relevant inpatient workup or three outpatient visits [11].
In recent years, inflammation of unknown origin (IUO) was introduced as an equivalent to FUO without fever, i.e. patients with normal temperature, but increased C-reactive protein (CRP) and/or erythrocyte sedimentation rate (ESR) on more than three occasions for more than three weeks and no diagnosis despite relevant inpatient or outpatient workup similar to FUO.
The overarching etiologies of FUO and IUO (i.e. infection, NIID, malignancies, and miscellaneous) are comparable [12,13,14,15,16], although infections are usually more prevalent in FUO and NIID more prevalent in IUO [17,18,19,20]. Therefore, the diagnostic approach is similar in both conditions [21]. It is important to remember that not all patients with unexplained infection or nonspecific systemic inflammation meet the stringent criteria of FUO or IUO, but they may still be suitable candidates for a [18F]FDG PET/CT exam.
Identification and accurate localization of the causes of FUO/IUO is essential to initiate appropriate treatment or to guide further diagnostic procedures [22]. Conventional radiology may be of limited use since infectious and inflammatory conditions often cause limited morphologic changes especially at early stages [12, 22]. [18F]FDG PET/CT has become the imaging modality of choice in the work-up of patients with FUO/IUO and has replaced scintigraphy with [67Ga]Ga-citrate or radiolabeled white blood cells if access to PET/CT is available [23]. The advantages of [18F]FDG PET/CT include the possibility to perform a whole-body examination in a single imaging session with good resolution and high sensitivity for detecting low-grade and early stage infection/inflammation with relatively lower radiation exposure compared to a diagnostic contrast-enhanced whole-body CT scan [5, 24, 25]. [18F]FDG PET/CT is superior to CT of the chest-abdomen-pelvis in reaching a final diagnosis in FUO; one study reported a diagnostic yield beyond conventional CT estimated at 32% [5], and one showed that [18F]FDG PET/CT performed three to four-fold better than CT with regards to diagnostic yield and clinical helpfulness [18]. The better performance has been explained by [18F]FDG uptake in the vascular regions [4] or inflammation of the musculoskeletal system [5] that are not easily detected by CT. One study suggests [18F]FDG PET/CT as first-line modality especially in FUO-patients with suspected endovascular infection, large vessel vasculitis, and hematological malignancy [26]. The nonspecificity of [18F]FDG uptake may be considered an advantage owing to the broad spectrum of differential diagnosis in FUO/IUO. On the other hand, the general limitations of false-positive [18F]FDG uptake, false-negative scans, physiologic uptake etc. also apply to infection and inflammation, which may lead to unnecessary invasive investigations or therapy.
The literature on [18F]FDG PET in FUO/IUO reflects the heterogeneous nature of the clinical entity itself and comparison across different studies is difficult. It may be difficult to dichotomize findings to obtain sensitivity and specificity, and instead, most studies report either “diagnostic yield” or the proportion of patients in whom FDG-PET/CT was considered “helpful”. However, both terms are defined differently; some consider only true-positive findings helpful, whereas some also include true-negative findings that may rule out focal infection, inflammation, or malignancies with a high negative predictive value. Some define the term “diagnostic yield” as the fraction of true positives among all positive and negative findings, whereas some the term interchangeably with diagnostic helpfulness [23, 27, 28].
. The eldest studies performed with stand-alone PET are now obsolete and not comparable to those performed with modern PET/CT scanners. Most studies are retrospective, with a significant heterogeneity with regard to the use of [18F]FDG PET/CT during the workup strategy, and baseline characteristics such as population size, definition of FUO/IUO, inclusion and exclusion criteria, patient demographics, and imaging parameters.
The purpose of this consensus document is to help the clinicians and nuclear medicine specialists involved in the management of patients with FUO/IUO to decide how and when to perform [18F]FDG PET/CT in this setting according to the current evidence.
Methodology (Systematic search of the literature)
To obtain an evidence-based consensus document, the EANM Inflammation & Infection Committee created a working group to perform a systematic search of the literature. The literature search was based on the PICO (Population or problem–Intervention–Comparator–Outcome) strategy. The population has been defined as “patients with FUO/IUO”, the intervention as “[18F]FDG PET/CT” and several outcomes were considered including scan protocol, diagnostic yield, impact on management, prognosis, and cost-effectiveness.
A systematic literature search was prepared using two bibliographic databases (PubMed/Medline and Cochrane library) from 2001 up to December 2023. A broad search string using a combination of key words related to elements of the PICO question and in particular the Problem (“fever” OR “pyrexia” OR “FUO” OR “IUO” OR “PUO”) and the Intervention (“FDG” OR “fluorodeoxyglucose” OR “PET”) was used. Cochrane library yielded no results; in PubMed the first retrieved report on PET/CT was from 2006. The complete PubMed search string is presented in Supplemental File 1. We extracted systematic reviews and meta-analyses on the topic of interest as we considered those to be the most relevant evidence-based documents. Furthermore, we extracted all relevant original papers on the subject. Finally, we manually perused the reference lists of all identified admissible papers to identify any further papers. The flowchart for paper selection is presented in Supplemental File 2. All systematic reviews/meta-analyses and original articles (excluding case reports) related to the role of [18F]FDG PET/CT in patients with FUO/IUO are listed in a Supplemental file 3 and form the basis of the information reported in this evidence-based document.
Pre-scan investigations
There is no established consensus on which investigations should be performed prior to [18F]FDG PET/CT scan, but the diagnostic workup of FUO/IUO usually begins with routine laboratory tests (including a complete blood count with differential, ESR, and CRP levels), whereas first-line imaging consists of chest X-ray and abdominal ultrasound [29]. More advanced invasive procedures or 3D-imaging modalities such as CT, MRI and/or [18F]FDG PET/CT may be guided by symptoms, clinico-biochemical findings, or the physicians preference and are usually considered second-line, with PET/CT usually being performed when first-line work-up is negative or when a final diagnosis is not established. The main recommendations from the literature regarding relevant pre-PET-scan investigations in FUO [7, 16, 19, 29,30,31,32,33,34,35,36,37,38,39,40,41,42,43] or IUO [14, 16, 19, 32, 33, 44,45,46] are summarized below.
Pre-scan laboratory tests
CRP is a well-established nonspecific marker of infection, inflammation, and malignancy with an essential role in clinical routine. CRP is elevated in most cases of prolonged fever, FUO and IUO, but the association between CRP thresholds and contribution of [18F]FDG PET/CT remains controversial. Several reports showed a significant association between CRP levels and prediction of usefulness [19, 29, 38, 44, 46,47,48,49,50,51], while others did not observe this relation [14, 34, 35, 37, 43, 52,53,54], and similar opposing results were encountered in pediatric patients [33, 41]. The majority of patients in the abovementioned reports had elevated CRP, but no cut-off value has been established to select patients for [18F]FDG PET/CT or to predict helpfulness. Some suggest the number of PET/CT positive patients increase with increasing CRP [14, 29], and some studies report that PET/CT-positive findings are very rare in patients with normal CRP-levels [45, 55], but there are also patients in some studies that are PET/CT positive despite normal CRP levels [34, 47].
Other pre-scan laboratory tests showed similar contradictory results: ESR [7, 31, 33, 35, 37, 44], leukocyte count [7, 33, 34, 41], platelets [5, 31], serum procalcitonin [11, 36], and hemoglobin [29, 31, 43]. One study suggested a positive association between the number of inflammatory markers, final diagnosis, and [18F]FDG PET/CT results [38]. In HIV-patients with FUO, controversy also remains whether a correlation exists between [18F]FDG uptake and HIV viremia [36, 56,57,58].
In conclusion, several pre-scan laboratory tests are routinely used depending on the clinical setting. However, their impact on [18F]FDG PET/CT yield is unclear and further studies are warranted especially aiming to establish a valid CRP cut-off in FUO (currently ranging from 7 to 50 mg/L). On the other hand, the yield or helpfulness of [18F]FDG PET/CT in the presence of normal or low CRP values is very low.
Pre-scan imaging
Some relatively simple and inexpensive diagnostic tests are still recommended as first-line for patients with FUO/IUO to separate relatively more apparent diseases from true FUO/IUO cases, but there is no consensus on which modality to employ. Some sugge st abdominal ultrasound and chest X-ray in low-resource areas, some suggest CT, and others suggest an imaging approach guided by symptoms and clinico-biochemical findings, but there is no firm evidence to support a standardized imaging strategy that should routinely precede [18F]FDG PET/CT [29, 59, 60].
Practical scan considerations
Generally, scan protocol and recommended administered [18F]FDG activity should adhere to existing EANM guidelines for tumour and infection imaging [61, 62].
Patient preparation
[18F]FDG administration should be preceded by fasting for at least 6 h. In patients with suspected cardiac pathology (e.g. endocarditis, cardiac sarcoidosis) a prolonged fasting is recommended for at least 12–24 h, in combination with a high-fat low-carbohydrate diet to ensure optimal suppression of physiological myocardial uptake. Supplemental intravenous low-dose unfractionated heparin (50 IU/kg 15 min prior to [18F]FDG administration) may also be considered especially in patients unable to complete long-term fasting and diet, e.g. diabetics [63]. Plasma glucose levels are recommended to be < 200 mg/dL (11 mmol/L). Even though the effect of hyperglycemia on [18F]FDG uptake is probably less pronounced on inflammatory cells compared to malignant cells [64], a recent study showed that the yield of FDG PET/CT in bacteremia of unknown origin was lower in patients with moderate to severe hyperglycemia compared to normoglycemic patients [65].
Pre-scan treatment with corticosteroids (e.g. prednisone, prednisolone, methylprednisolone) is known to reduce uptake in inflammatory cells and hampers [18F]FDG PET/CT helpfulness in inflammatory conditions like vasculitis and polymyalgia rheumatic [66, 67]. Thus, corticosteroids may negatively influence the outcome of [18F]FDG PET/CT in FUO [34]. Treatment for longer than 3 days may significantly reduce [18F]FDG uptake in vasculitis [67], whereas 8 weeks treatment significantly reduced sensitivity in polymyalgia rheumatic [66]. In the latter study, one week of tapering followed by one week of discontinuation significantly increased sensitivity again but, generally speaking, there is no established lower limit in the literature. Corticosteroids should be reduced to a minimum or temporarily withdrawn, especially when vasculitis is suspected. Despite the few available results with doses of 15–60 mg [64, 68], a pragmatic recommendation is to postpone scans in patients treated with doses higher than 15 mg for > 3 days to reduce the risk of false-negative findings.
In contrast to glucocorticoids, the impact of antibiotic treatment is less well-known in the setting of FUO/IUO. Data from one study on [18F]FDG PET/CT in bloodstream infections reported a reduced possibility to find the focus of infection after more than one week of antibiotics with a further drop with increasing duration of treatment [69]. One study in FUO patients reported that empiric antibiotic therapy is associated with non-contributory [18F]FDG PET/CT [29], whereas others did not observe any association [38, 40, 70].
In conclusion, the effect of hyperglycemia is probably less pronounced than in cancer work-up, but plasma glucose levels are still recommended to be < 200 mg/dL (11 mmol/L) and thorough patient preparation is especially important if a cardiac focus is suspected. PET/CT is not recommended in patients under glucocorticoid treatment > 15 mg for more than 3 days, but scans can be performed despite pre-scan antibiotic treatment.
Protocol
A major advantage of [18F]FDG PET/CT over CT, MRI and ultrasound is the possibility to screen the whole body in patients with suspected systemic disease and few diagnostic clues. The scan field should minimally include the vertex to mid-thighs, but a total-body acquisition could be considered.
Stand-alone PET is nowadays considered obsolete in FUO and only combined [18F]FDG PET/CT will be addressed in this document A disadvantage of hybrid-PET/CT over CT alone is the higher combined radiation exposure [71], which should be kept as low as possible especially in children and young adults [33]. Depending on the clinical indication, CT may be contrast-enhanced or non-enhanced [41]. The latter is often referred to as low-dose, although this may be misleading, and the actual settings are usually based on local practice more than guidelines. Adding CT to PET results in an additional exposure of approximately 2–10 mSv depending on protocols on top of the radiation exposure of FDG (0.019 mSv/MBq). In the literature on FUO, most studies used a non-enhanced “low-dose” CT [14, 18, 19, 29, 32, 33, 37, 38, 40, 44, 45, 48,49,50, 52, 54, 69, 72,73,74] while few studies were performed with contrast-enhanced CT [26, 39, 44, 48, 51, 69, 75]. However, head-to-head comparisons are lacking to determine the incremental value of upfront contrast-enhanced CT. Solid malignancies and abscesses are notable exceptions, and if these are suspected upfront, contrast-enhanced CT is indicated but may be performed in a separate setting.
In conclusion, a non-enhanced “low-dose” CT is sufficient in FUO/IUO to define the location of metabolic abnormalities that could lead to the diagnosis. There is usually limited value of contrast-enhanced CT because of the often relatively minor morphologic changes from infectious and inflammatory processes, especially at early stages.
Interpretation and reporting
Interpretation and reporting is similar to [18F]FDG PET/CT scans for tumor imaging and non-oncological indications. The interpretation is primarily based on a visual assessment whereas only limited and heterogeneous data is available on semi-quantitative interpretation criteria [16, 20, 39, 76,77,78]. Findings may be focal (e.g. abscesses, endocarditis), diffuse (e.g. colitis, large vessel vasculitis), or confined by anatomic structures (e.g. spondylodiscitis, graft material). Some physiologic, reactive [18F]FDG-activity is often seen diffusely around implants but it is usually not difficult to distinguish this uptake from pathologic activity characterized by a heterogeneous/multifocal pattern. In patients with metallic or prosthetic implants, non-attenuation corrected PET images are helpful to distinguish true uptake from artefacts. Focal [18F]FDG uptake is more typical for infection than diffuse low-grade uptake. Finally, scans may display indirect signs of infection and inflammation, e.g. diffuse uptake in the bone marrow and spleen [16].
Overall diagnostic yield
Due to the heterogeneity of potential diagnoses, a lack of well-defined reference standards, and many cases without a final diagnosis, the classical approach of determining the diagnostic performance of a test by reporting its sensitivity, specificity and predictive values may not be the most appropriate method. The majority of studies consider only true positive [18F]FDG PET foci as helpful, i.e. those that directly lead to a diagnosis. True negative findings are rarely included, even though patients with a negative [18F]FDG PET/CT usually are more likely to show a spontaneous clinical regression or remission [38, 44, 75, 79,80,81]. Secondly, true negative scans indicate a potential to reduce additional futile imaging, which contributes to the cost-effectiveness of [18F]FDG PET/CT when performed early in the diagnostic workup [3, 22]. On the other hand, studies also reported false positive findings in as many as 26–33% of patients that may lead to subsequent additional examinations [19, 35, 38, 43, 74, 82]. Importantly, a significant proportion of FUO/IUO patients (7–47%) remains without a final diagnosis after [18F]FDG PET/CT.
Even though many studies report sensitivities and specificities of [18F]FDG PET/CT in the context of FUO/IUO, the terminology of diagnostic yield or helpfulness is a better parameter, i.e. the proportion of all PET scans that help the clinicians in subsequent patient management [23, 27, 28].
Several meta-analyses have demonstrated the usefulness of [18F]FDG PET/CT in reaching the final diagnosis of FUO/IUO with a diagnostic yield of 56–60%, which is at least 30% higher than conventional CT, and a significantly better association between negative scans and spontaneous remission (Table 1) [3,4,5,6, 12, 22, 83]. Regarding the latter, a recent meta-analysis reported a significantly higher cumulative incidence of spontaneous remission of 20–78% in patients with negative [18F]FDG PET/CT results compared to 0–48% in those with positive results [6]. [18F]FDG PET/CT is also superior to [18F]FDG PET alone and other nuclear imaging methods such as [67Ga]Ga-citrate or leukocyte scintigraphy [22, 83]. Besides mere diagnostic yield, Besson et al. also reported that abnormal [18F]FDG uptake is associated with a statistically significant higher rate of definitive diagnoses compared to normal scans (83% vs. 36%) with a pooled odds ratio of 8.94 [3]. Other than the general FUO/IUO populations, two additional meta-analyses were identified in specific subpopulations. One on intensive care unit (ICU)-patients reported that [18F]FDG PET/CT is equally clinically helpful in the ICU-setting, i.e. in 65% of patients [84]. The one on paediatric patients did not assess diagnostic yield per se, but concluded that PET-positive patients were significantly more likely to receive a final diagnosis compared to normal scans (odds-ratio 17) [85].
The literature search identified 49 relevant clinical studies on the diagnostic value of [18F]FDG PET/CT in adult patients with FUO/IUO [13,14,15,16,17,18,19,20, 26, 29, 32, 34, 35, 37,38,39, 43,44,45,46,47,48,49,50,51,52, 54, 55, 72, 74,75,76,77,78,79,80,81,82, 86,87,88,89,90,91,92,93,94,95,96]; an overview is presented in Table 2. Most of the clinical studies were retrospective single centre cohorts (n = 34, 69%) with large variation in sample size (12–524 cases). Most studies included only patients with FUO (n = 30, 61%), while fourteen studies included patients with a case-mix of FUO/IUO (29%), and five studies evaluated only patients with IUO (10%). All included studies focused on diagnostic or clinical value of [18F]FDG PET/CT in FUO or IUO patients, but two studies also investigated cost-effectiveness [76, 86], and two studies compared [18F]FDG PET/CT with [67Ga]Ga-citrate scintigraphy [81, 90]. Final diagnosis was related to infection in 10–68% patients, NIID in 8–60% patients, malignancy in 3–36% patients and a variety of uncommon conditions in 2–31% patients. Helpfulness of [18F]FDG PET/CT in the diagnosis or management of FUO ranged from 19 to 96% with higher values when both true positives and true negatives were considered. In some studies, [18F]FDG PET/CT was deemed essential in 6–26% of patients to reach a final diagnosis [26, 29, 32, 37, 75, 78] because no other investigation, including CT of chest and abdomen, was able to establish a diagnosis. With the highly variable populations and sample sizes in the available literature, there is a significant risk of selection bias.
Balink et al. performed the largest multicentre retrospective study on FUO/IUO patients (n = 498) [13]. [18F]FDG PET/CT had a high diagnostic accuracy (89%) and the addition of [18F]FDG PET/CT to a model for the prediction of a diagnosis including CRP, ESR and age resulted in a significant change in patient classification in 42% of patients.
The largest prospective study (n = 524) on the diagnostic value of [18F]FDG PET/CT in patients with FUO aimed to develop a diagnostic model to distinguish the different causes of FUO [76]. [18F]FDG PET/CT showed positive findings in 477 (91%) patients (diffuse or focal high uptake in various organs and tissues). The diagnostic model including [18F]FDG PET/CT and relevant clinical parameters (e.g. blood cell counts, inflammatory and immunological indicators, age) showed a good performance in discriminating the cause of FUO with AUCs for infection, malignancy, and NIID of 0.88, 0.93 and 0.95, respectively. Previous studies have also divided positive [18F]FDG PET/CT studies into focal and nonspecific abnormal uptake [15, 16]. The latter is represented by diffuse high [18F]FDG uptake of spleen and bone marrow and multiple lymph nodes with high [18F]FDG uptake and symmetrical distribution. This pattern was considered non-contributing to the diagnosis or even false positives in other studies [16, 19, 80, 82, 89]. However, nonspecific abnormal [18F]FDG uptake as well as a negative [18F]FDG PET/CT scan could also be of benefit for the patients.
The variable performance of [18F]FDG PET/CT in FUO/IUO may be explained, as previously described, by a multitude of factors; the complexity of patients, definitions of FUO/IUO, retrospective and observational study designs, relatively small sample sizes, differences in pre-scan work-up, differences in [18F]FDG PET/CT timing, and varying definitions of a clinical helpful result.
Overall, the results of most studies show that a positive [18F]FDG PET/CT is often contributive and, in some cases, is essential to establish a diagnosis by identifying potential causes of FUO/IUO, localizing sites for further evaluation, and guiding further management. Conversely, a negative scan excludes focal disease and predicts a favourable prognosis.
Diagnostic yield in specific populations
As mentioned above, [18F]FDG PET/CT provides a good diagnostic yield in the general population of adults with FUO/IUO and can be considered as a primary imaging tool. In addition to the general adult population, [18F]FDG PET/CT has also been evaluated in specific subpopulations with FUO/IUO, including children, intensive care unit patients, patients with end stage renal disease, and HIV (Table 3).
Children with FUO/IUO
Six retrospective studies (n = 238 patients) evaluated the value of [18F]FDG PET/CT in children with FUO/IUO, including one study in pediatric transplant patients [33, 41, 97,98,99,100]. The largest study by Pijl et al. including 110 children with FUO showed that [18F]FDG PET/CT identified a true positive cause of fever in 53 (48%) children, and in 58 children (53%) treatment modifications were based on PET/CT results. The sensitivity and specificity were 86% and 79%, respectively, and CRP levels were positively associated with finding a true focus [41]. [18F]FDG PET/CT was considered helpful in 48%, whereas 38% remained without a final diagnosis after [18F]FDG PET/CT [33, 98, 100]. In addition and similar to the adult population, the same issues were encountered regarding different definitions of helpful and whether or not negative scans were considered helpful, non-contributory or unclassified [33, 97, 100]. The clinical helpfulness across the six studies had a considerable span but with sample sizes ranging from 5 to 110 patients, the relative weight of these results are different and not readily comparable.
Patients in the ICU
Only one prospective study on the use of [18F]FDG PET/CT in critically ill, mechanically ventilated patients admitted to the ICU with FUO/IUO is available. The study reported that 21/35 scans (60%) were true positive, 11/35 scans were true negative, and three scans were considered false positive resulting in a sensitivity of 100%, specificity of 79% and overall accuracy of 91%. The authors emphasized that, besides the high accuracy, a normal [18F]FDG PET/CT scan was also considered important, since it ruled out infections requiring prolonged antibiotic therapy or drainage [101].
Patients with end-stage renal disease
Two retrospective studies evaluated the role of [18F]FDG PET/CT in FUO patients suffering from end-stage renal disease on renal replacement therapy. The first study evaluating 20 patients (18 on hemodialysis, two on peritoneal dialysis) showed active lesions in 15 patients, and negative scan results in five patients. In all but one patient, imaging results led to a change in treatment [102].
In the second study, 46 patients underwent [18F]FDG PET/CT (21 on hemodialysis, 8 on peritoneal dialysis, and 17 renal transplants). Twenty-nine scans showed at least one focus of increased uptake, 17 scans turned out to be negative and [18F]FDG PET/CT was helpful in identifying the cause of FUO in 22 patients (48%). CRP and procalcitonin levels were significantly higher in patients with a helpful [18F]FDG PET/CT scan [40].
Patients with HIV
One study prospectively evaluated the performance of [18F]FDG PET/CT in 20 HIV-infected patients with FUO in comparison to 10 HIV-infected high viraemic patients without FUO. Despite the limited number of included patients, high viraemic status did not interfere with a correct scan interpretation but different uptake patterns were observed: more peripheral active lymph nodes in patients without FUO compared to more central active lymph nodes in FUO patients. [18F]FDG PET/CT contributed to the diagnosis or exclusion of a focal etiology in 80% of the patients. The absence of active central lymph nodes in FUO patients showed a 100% negative predictive value for focal disease. Lymph node biopsy in central active areas allowed identification of underlying disease in all patients with FUO. Furthermore, [18F]FDG PET/CT demonstrated more extensive disease than conventional imaging [36]. The other study in this patient population found [18F]FDG PET/CT helpful in 9/10 patients, six with infection and three with malignancy [103].
In conclusion, [18F]FDG PET/CT can be considered useful for evaluating the cause of FUO/IUO in these specific populations, taking into account the same caveats as the general adult FUO/IUO population. The diagnostic yield and helpfulness of [18F]FDG PET/CT in these specific patient groups are similar to the results in the general adult population.
Impact on patient management and prognosis
A correct and early diagnosis can change the therapeutic strategy, i.e. initiate new therapy, modulate already instituted therapy, or switch therapy regimen completely. Moreover, it may guide specific invasive and noninvasive procedures such as biopsy or drainage, specific serology, or cultures of blood, urine, or tissues with a direct impact also on costs [55].
A major contribution of [18F]FDG PET/CT for obtaining the final histological diagnosis is to guide the clinician to the most appropriate and accessible site for biopsy to confirm the underlying etiology [72].
An indirect impact is to exclude several causes and to narrow down the range of possible diagnoses. About 43–75% of adult patients with undiagnosed FUO experience spontaneous remission of fever before reaching a final diagnosis [7, 104], and empirical treatment with corticosteroids or nonsteroidal anti-inflammatory drugs does not affect this rate. Identifying predictors of spontaneous resolution could reduce the use of unnecessary, invasive tests or empirical treatments, and furthermore potentially reduce patient anxiety. As such, a negative PET/CT result can be a good predictor of favorable prognosis in patients with undiagnosed FUO after a series of unsuccessful investigations; watchful waiting may be a valid option for undiagnosed FUO patients with no specific findings. One systematic review studied the association of [18F]FDG PET/CT results with spontaneous remission in FUO. Patients with negative scan results were significantly more likely to have spontaneous remission of fever than were those with positive scan results, with a summary risk ratio of 5.6 (95% CI, 3.4–9.2) [6]. This may also have a direct impact on patient outcome, as prognosis was generally good and mortality very low in patients in whom a final diagnosis could not be obtained [105,106,107].
As FUO is caused by a wide variety of diseases; the overall prognosis highly depends on the underlying disease [8], with malignancy probably having the most prominent association with mortality [108,109,110].
However, although promising, more robust evidence is required to evaluate the prognostic role of [18F]FDG PET/CT in FUO/IUO patients.
Cost-effectiveness
An important aspect of any imaging strategy is cost, and to date, few studies assessed the cost-effectiveness of [18F]FDG PET/CT in FUO/ IUO reporting that [18F]FDG PET/CT is cost-effective in specific scenarios of FUO/IUO. Beccera-Nakayo et al. included 20 FUO-patients that underwent a scan after a mean hospital stay of 28 days. They registered all costs in the FUO-process including hospitalization and diagnostic procedures prior to PET/CT. They found a potential cost reduction of 5,471 € (49%) if [18F]FDG PET/CT was performed earlier [86]. Balink et al. found similar results in 92 IUO-patients, 46 who did not undergo [18F]FDG PET/CT (group A) and 46 who underwent [18F]FDG PET/CT (group B). Costs in group B were reduced with 5.298 € (42%) compared to group A, and at the same time a definite diagnosis was reached in more than twice the patients, i.e. 32/46 in group B versus 14/46 in group A [111]. In the largest and most recent study, Chen et al. included 741 FUO/IUO-patients; 44% underwent [18F]FDG PET/CT They did find higher overall costs, more additional tests and longer hospitalization in the [18F]FDG PET/CT-group compared to controls. However, this population was older and had more critically ill patients, and again the number of definite diagnosis was significantly higher in the intervention group. Furthermore, the total costs and hospitalization stay was reduced if [18F]FDG PET/CT was performed within 7 days [88].
Recommendations
Conclusions
FUO/IUO remains a clinical challenge due to the heterogeneous patient presentation, a wide variety of differential diagnoses, and the lack of an established workup strategy. The literature is as challenging and heterogeneous as the population, which hampers pooling of data and direct comparison between studies.
However, [18F]FDG PET/CT has a definite role in the diagnostic workup with an overall diagnostic yield/helpfulness of 50–60%. A positive scan is often contributory and, in some cases, even essential to diagnosis, whereas a negative scan may be equally important as it excludes focal disease and predicts a favorable prognosis. Similar results are obtained in specific populations such as ICU-patients, children and HIV-patients.
Data availability
All data generated or analysed during this study are included in this published article [and its supplementary information files].
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All authors contributed to the study conception and design. Material preparation, data collection and analysis were performed by Soren Hess, Edel Noriega-Alvarez, Lucia Leccisotti, Giorgio Treglia, Domenico Albano, Anne Roivainen, Andor Glaudemans and Olivier Gheysens. The first draft of the manuscript was written by Soren Hess and all authors commented on previous versions of the manuscript. All authors read and approved the final manuscript.
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Hess, S., Noriega-Álvarez, E., Leccisotti, L. et al. EANM consensus document on the use of [18F]FDG PET/CT in fever and inflammation of unknown origin. Eur J Nucl Med Mol Imaging 51, 2597–2613 (2024). https://doi.org/10.1007/s00259-024-06732-8
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DOI: https://doi.org/10.1007/s00259-024-06732-8