Abstract
Primitive malignant renal tumours comprise 6% of all childhood cancers. Wilms tumour (WT) or nephroblastoma is the most frequent type accounting for more than 90%. Imaging alone cannot differentiate between these tumours with certainty but it plays an important role in screening, diagnostic workup, assessment of therapy response, preoperative evaluation and follow-up. The outcome of WT after therapy is excellent with an overall survival around 90%. In tumours such as those where the outcome is extremely good, focus can be shifted to a risk-based stratification to maintain excellent outcome in children with low risk tumours while improving quality of life and decreasing toxicity and costs. This review will discuss the imaging issues for WT from the European perspective and briefly discuss the characteristics of other malignant renal tumours occurring in children and new imaging techniques with potential in this matter.
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Introduction
Primitive malignant renal tumours comprise 6% of all childhood cancers. Wilms tumour (WT) or nephroblastoma is the most frequent type accounting for more than 90% [1]. All other malignant renal tumours occurring in children such as clear cell sarcoma, rhabdoid tumour and renal cell carcinoma are rare.
Imaging alone cannot differentiate between these tumours with certainty but it plays an important role in screening, diagnostic workup, assessment of therapy response, preoperative evaluation and follow-up. Abdominal US with colour Doppler, chest radiograph, CT and MRI are commonly used for anatomical staging and detection of metastases. New techniques such as 18F-fluorodeoxyglucose positron emission tomography (FDG-PET) CT and diffusion-weighted imaging (DWI) with MRI are being evaluated for their potential value in the imaging strategy of malignant renal tumours in adults and children.
The outcome of WT after therapy is excellent with an overall survival around 90% [1]. In tumours such as those where the outcome is extremely good, focus can be shifted to a risk-based stratification to maintain excellent outcome in children with low risk tumours while improving quality of life and decreasing toxicity and costs. At the same time it is important to identify the small group of children with high risk tumours who might benefit from intensified therapy. In this strategy, care should be taken not to increase the burden of invasive or ionizing diagnostic investigations in all children [2].
The therapeutic approach for WT in Europe is different from that in the United States [3, 4]. This review will discuss the imaging issues for WT from the European perspective and briefly discuss the characteristics of other malignant renal tumours occurring in children and new imaging techniques with potential in this matter.
Wilms tumour
Differential diagnosis
In Europe, WT is treated according to the Société Internationale d’Oncologie Pédiatrique (SIOP) 2001 trial and study protocol [5]. Since biopsy is not required in this protocol, renal tumours with features matching WT are treated accordingly. The diagnosis will be confirmed on pathological examination after preoperative chemotherapy and surgery. The advantages of preoperative chemotherapy have been extensively published in various papers. Analysis of the SIOP-9 study showed that in only 2% of children preoperative chemotherapy was given inappropriately for benign lesions and in 3% for other malignant lesions [6]. This seems acceptable since preoperative chemotherapy of short duration (4 weeks) with vincristine and actinomycin-D is not associated with long-term complications and is also effective in most non-Wilms tumours. Vujanic et al. [7] reported the results of pre-treatment needle biopsies in children with non-metastatic renal tumours. In 84% the diagnosis of WT was confirmed and in 12% it revealed either an alternative renal malignancy or neuroblastoma. In 4% the specimen was not diagnostic and in 2% significant complications were described. Whether the pathological information provided by biopsy before therapy is worth the possible complications is not yet proved.
Sometimes a neuroblastoma invading the kidney can mimic a WT. The presence of calcifications and the typical encasement of vessels are signs in favour of neuroblastoma. Elevation of catecholamine levels in 24 h urine studies will confirm the diagnosis in more than 90% [8]. Meta-iodobenzylguanidine (MIBG)-Iodine123 radiotargeting can be very helpful in this situation (Fig. 1).
Imaging at diagnosis
The initial treatment consists of chemotherapy. This will reduce tumour size, hence facilitating subsequent surgery and lowering the risk of intra-operative tumour rupture. Pre-operative chemotherapy will also downstage tumours and reduce postoperative therapy. Clinical history, physical examination and diagnostic imaging will assist in differentiating WT from other renal pathology, either benign or malignant. Needle biopsy is recommended in cases of unusual clinical presentation (age above 6 years, urinary infection, septicaemia, psoas inflammation) or unusual imaging findings for WT (calcification, voluminous lymph nodes, renal parenchyma not visible, almost entirely extrarenal mass).
Furthermore, imaging will depict the locoregional extension, metastatic spread and contralateral disease.
Initial imaging should consist of abdominal US with colour Doppler and chest radiograph in 2 projections; frontal and lateral view. Depending on the size and extension of the tumour and the expertise of the radiologist, complementary abdominal contrast-enhanced CT or MRI will be required to further delineate tumour extension and exclude bilateral disease with certainty (Fig. 2). Although CT is more readily available and faster, MRI is the preferred technique since it does not use ionizing radiation, even though general anaesthesia or sedation is usually necessary in these young children. If there are suspicious pulmonary lesions on chest radiograph, additional chest CT is recommended.
The primary tumour
WT presents as a large spherical mass, with a mainly intrarenal localization. The tumour can be solid and homogeneous but is usually heterogeneous with areas of haemorrhage, necrosis or cysts. In <15% the tumour contains calcifications. The remaining normal kidney tissue can be difficult to detect but is often stretched at the periphery of the tumour (Fig. 3). US is an excellent technique to assess the movement of the mass in relation to its surroundings in order to exclude invasion or adherence to adjacent organs. Measurement of the tumour in three planes is required. If the tumour is large and difficult to delineate from the kidney, kidney and tumour is measured as one. On CT and MRI the tumour enhances less than normal renal tissue making it more conspicuous.
The contralateral kidney
Whenever a renal tumour (presumably a WT) is detected, the contralateral kidney should be examined for synchronous bilateral disease that occurs in 5% of children. Bilateral disease comprises bilateral WT or bilateral nephrogenic rests (NRs) (nephroblastomatosis) and/or WT. Other lesions may mimic bilateral disease, including lymphoma, leukaemia or polycystic kidney disease (Fig. 4). Bilateral disease upstages the patient to stage V [5]. The aim of treatment then becomes to cure and at the same time preserve as much functional renal tissue as possible by using parenchyma-sparing surgery. Preoperative imaging will then play a crucial role in determining the possibilities of partial nephrectomy.
In case of detection of other non-malignant abnormalities of the other kidney endangering the renal function (e.g. dysplasia, hydronephrosis) or absence of the other kidney, partial nephrectomy must also be considered.
Bilateral disease occurs more frequently in children with NRs in their kidneys. NRs are clusters of embryonal nephroblastic cells that can persist into childhood and have the potential to transform into a malignancy [9]. This makes detection of these often small lesions important. Rohrschneider et al. [10] compared the sensitivity of US, CT and MRI to detect macroscopic NRs and concluded that US is less sensitive than CT and MRI. The value of high-resolution US techniques such as tissue harmonic imaging has not yet been evaluated. Nowadays, surgeons no longer explore the contralateral kidney before nephrectomy since imaging is sufficiently capable of detecting small lesions in the contralateral kidney [11, 12]. Differentiating benign NRs from WT is important for it will obviously determine the appropriate management. MRI shows distinctly different characteristics on pre-contrast T2-weighted images between sclerotic and hyperplastic NRs and WT. This might help in decision making about continuation of chemotherapy or partial nephrectomy [13]. This is particularly useful since pathological examination of a small biopsy specimen cannot discriminate with confidence between benign NRs and WT (Fig. 5).
The management of bilateral disease is still one of the most challenging issues in WT especially when nephron-sparing surgery is not possible due to the location of the lesions.
The rest of the abdomen
Enlarged lymph nodes are frequently encountered in the region of the tumour. Imaging studies are unable to differentiate between reactive nodes or tumour positive nodes. Hence lymph node biopsies will be performed during surgery, according to the protocol.
WT can metastasise to the liver in 15–20% of children making meticulous inspection of the hepatic parenchyma necessary.
Although rare, tumour rupture is a major risk factor for abdominal relapse. The reason for preoperative chemotherapy in the SIOP protocol is to decrease the risk of intraoperative tumour rupture, that would upstage the patient to stage III (Table 1). These children will then receive abdominal radiotherapy as part of their postoperative treatment if the tumour shows intermediate or high risk histology. In the SIOP protocol, the local stage is determined by pathological examination of the nephrectomy specimen. However, clinical signs and imaging could also suggest rupture. In the current protocol these findings are not taken into account for the final local staging. Brisse et al. [14] demonstrated from a retrospective study of 57 patients with either clinical and/or CT signs of rupture that detailed analysis of abdominal CT scans may distinguish intraperitoneal from retroperitoneal ruptures. These imaging findings are not always coupled with clinical signs. They suggested that diagnostic features of intraperitoneal rupture should be considered as stage III regardless of other postoperative pathological criteria. On the other hand, they found no increased risk for abdominal relapse in children with isolated retroperitoneal rupture who did not receive abdominal radiotherapy. These findings encourage the possible need to value imaging findings of both retroperitoneal and intraperitoneal rupture when considering postoperative treatment, to prevent respectively over- and under treatment of these children.
Small amounts of non-haemorrhagic peritoneal fluid should not be considered as a sign of rupture: it can correspond to a peritoneal inflammatory reaction to rapid tumour growth or be due to inferior vena cava (IVC) compression or thrombosis [3].
In 4–10% of children the tumour extends into the IVC [15]. Preoperative chemotherapy will usually at least decrease the size of the tumour thrombus and possibly even induce resolution of the IVC extension. This will reduce the risks of massive haemorrhage or pulmonary embolus during surgery. US in combination with colour Doppler studies is the most reliable modality to examine the patency of the IVC (Fig. 6) [16].
The lungs
Lung metastases are present in 15–20% of children with WT. In the current SIOP protocol chest radiograph (CXR) (AP or PA and lateral view) is still the basic imaging tool to exclude pulmonary metastases. Complementary chest CT is recommended only in cases of distinct or suspicious lesions on CXR [5]. In North America, CT has become the routine method of diagnosis for assessment of pulmonary lesions since it is widely accepted that chest CT is a more sensitive technique for detecting pulmonary nodules than conventional radiographs. However, CT cannot differentiate between small benign pulmonary lesions (that frequently occur in children) and metastases [17–19]. Moreover, it has not been proven that detecting smaller lesions at diagnosis (and possibly also benign lesions) will improve the outcome of WT patients [18, 20–22]. The ongoing discussion around the dilemma between using the most accurate imaging technique to detect pulmonary lesions and avoiding overtreatment in children with a very good overall prognosis has been recently summarized by Owens et al. [3, 23, 24]. In the current SIOP protocol a special clause is made for patients with lung lesions detected on chest CT and not on CXR. These lesions are called CT-only lung metastases. The SIOP protocol proscribes that these lesions should be ignored and the patients with CT-only nodules should be treated as if without lung metastases (double agent instead of three-drug chemotherapy and no lung irradiation). One of the aims of the study is to evaluate the outcome of these patients with CT-only metastases. If it is not different from patients without CT-only lesions, with same stage and histology, it could make detection of these lesions unnecessary and hence chest CT redundant at diagnosis. It will also prevent these patients from receiving more toxic treatment with more long-term side effects. If on the other hand, patients with CT-only metastases do worse, chest CT should undoubtedly become the mandatory diagnostic tool in the imaging strategy of WT.
Preoperative imaging
Most tumours decrease in size during preoperative chemotherapy and/or show changes in appearance indicating necrosis. The tumour rarely increases in size (5%), predicting poorer event-free and overall survival [25]. The surgeon needs to know the extent of the tumour, its location within the kidney and its relation to the central vessels, diaphragm, liver, spleen, pancreas and adrenal glands before operation. Enlarged lymph nodes, intra-abdominal metastases (mainly liver) and thrombus in renal vein, IVC or right atrium must be looked for. US is often sufficient to answer these questions and in difficult cases it is recommended to perform the examination in the presence of the surgeon. If US does not provide satisfactory information, MRI is the preferred complementary modality because of the lack of ionizing radiation.
Kidney-sparing surgery is indicated in cases of bilateral disease, underlying urologic or nephrologic disease (e.g. horseshoe kidney, single kidney) or genetic syndromes with an increased risk of WT. In this context multiplanar acquisitions with MRI are extremely helpful in depicting the surgical possibilities and margins. Partial nephrectomy can also be considered in cases of simple unilateral disease; the SIOP protocol mentions contraindications for this procedure [26]. Some of these can be detected by the radiologist: tumour infiltrating into extrarenal structures, intra-abdominal metastases or enlarged lymph nodes, thrombus in the renal vein or IVC, tumour involving more than 1/3 of the kidney, multifocal tumour, central location and involvement of calyces.
Intraoperative US may also assist in defining the tumour margins more accurately.
Follow-up
Tumour relapse in WT is infrequent and typically occurs in the first 2 years after therapy. Considering the overall good prognosis of WT, imaging after treatment should also be minimally invasive and minimally harmful. Since recurrence of WT can be cured, it is important to detect it (Fig. 7). Children are followed with CXR and abdominal US. Abdominal US is recommended at a higher frequency in cases of metastatic disease in complete remission, if nephrogenic rests are present, in cases of bilateral disease and after partial nephrectomy, than for children with non-metastatic disease at diagnosis. There is no evidence or consensus about the frequency of follow-up studies.
Screening
Most WT occur in otherwise healthy children. A small number occur in children with genetic syndromes. Scott et al. [27] have produced guidelines for WT surveillance based on a review of current practice and available evidence. In summary, they recommend using renal US every 3–4 months until 5 or 7 years of age to screen children with a risk of developing WT >5%, depending on the syndrome. These children should first be offered a review by a clinical geneticist and detected lesions should be managed at a specialist centre.
Other renal malignancies of childhood
Clear cell sarcoma
Clear cell sarcoma of the kidney (CCSK) occurs in children with a peak age of incidence similar to that of WT. They account for approximately 4% of childhood renal tumours. Metastatic spread is wider than in WT; to bone, brain, liver, lymph nodes and lungs, in some cases long after nephrectomy. Radioisotope bone scan (99 m-Technetium-methylene diphosphate), MRI of the brain and chest CT are recommended for staging. Children with CCSK are at risk for relapse for a longer period of time than WT and they have a poorer outcome with long-term survival rates of 60–70% [1]. Imaging studies cannot distinguish between CCSK and WT (Fig. 8) [1, 28].
Rhabdoid tumours of the kidney
Rhabdoid tumours of the kidney (RTK) account for 1–2% of renal malignancies in childhood. RTK is a highly aggressive entity occurring exclusively in children and mainly in infants. Brain metastases or synchronous primary intracranial masses are often present at diagnosis. The brain lesion is usually near the midline and often in the posterior fossa. Survival is often <1 year from diagnosis. Imaging studies demonstrate a large, centrally located, heterogeneous soft-tissue mass involving the renal hilum. The appearance may closely resemble WT but subcapsular fluid collections, tumour lobules separated by areas of necrosis or haemorrhage and linear calcifications outlining tumour lobules can suggest the diagnosis of RTK. Renal vein invasion is common. RTK can metastasise to lungs, liver and brain [28, 29].
Renal cell carcinoma
Renal cell carcinoma (RCC) is the most common renal tumour in adults. It presents very rarely in childhood (1%). Children with tuberous sclerosis or von Hippel-Lindau disease or prior chemotherapy for cancer are at risk [30]. There also seems to be a higher incidence in children who have been previously treated for neuroblastoma [31]. Compared to WT, RCC more often presents bilaterally and is more likely to metastasize to bone. Calcifications are more frequently seen than in WT [28].
In contrast to adults, locoregional nodal spread seems not to worsen the prognosis [32].
Renal medullary carcinoma
Renal medullary carcinoma is a highly malignant tumour of epithelial origin occurring almost exclusively in adolescents and young adults with sickle cell trait or sickle cell disease, but not homozygous sickle cell disease [33, 34]. The age range at presentation is 10–39 years (mean age 20). Imaging shows a centrally located infiltrative lesion invading the renal sinus. The tumour is heterogeneous and hypovascular. Intratumoural and subcapsular haemorrhage are common. Calcifications have not been described. Renal vein thrombosis or encasement is a common feature [35]. The tumour metastasises to lungs and liver and responds poorly to chemotherapy or radiation therapy with a mean survival of 15 weeks from diagnosis.
Congenital mesoblastic nephroma
Congenital mesoblastic nephroma (CMN) is the most common solid tumour in the newborn. Below the age of 3 months, 72% of renal tumours are CMN. At 6 months this percentage decreases to 16% [36]. Although it used to be considered a congenital WT, it is now known to be a distinct entity. It is usually detected within the first 3 months or at least first year of life. Some cases are identified prenatally. Imaging studies demonstrate a large solid intrarenal mass that typically involves the renal sinus. It may contain cystic, haemorrhagic and necrotic components. Local infiltration of the perirenal tissues is common. Nephrectomy alone with a wide surgical margin is usually sufficient for cure. Local recurrence and spread to lungs, brain or bones is rare [28].
Primitive neuroectodermal tumour
Primitive neuroectodermal tumour (PNET) of the kidney is an extremely rare malignant tumour often presenting in an advanced stage. Renal PNET behaves more aggressively than PNET at other sites. It has poor response to chemotherapy. Imaging studies show an infiltrative mass that may present with calcifications and areas of necrosis. The tumour can extend in the renal vein or IVC [37, 38].
New imaging techniques
FDG-PET
FDG-PET has been established for a number of diseases in adults. In combination with CT the increased metabolic activity can be anatomically localized and hence provides more accurate information for staging; differentiating benign from malignant disease and monitoring response to treatment.
The applications in children are being further explored and are promising in many areas. Although PET-scanning is noninvasive, it does involve exposure to ionizing radiation and the total dose is significant, usually around 10 mSv. Uptake of FDG by WT has been described but a definitive role has not been established. For differentiating lung metastases from benign pulmonary lesions PET-CT fails since both conditions may involve increased glucose metabolism. Furthermore, the current resolution of PET-CT does not allow detection of micrometastases [39].
In a study by Misch et al. [40] 12 children with WT were examined with FDG-PET. Their results suggest that the usefulness of this technique could lie not in initial staging but in post-therapeutic imaging, non-invasive tumour characterisation and restaging in cases of recurrent disease.
Normal excretion of FDG through the kidney can be a limiting factor in detection of small renal tumours.
Quantitative MRI
DWI has been widely accepted as a powerful imaging technique in neuroradiology. With advances in MRI technology, diffusion-weighted sequences can now also be used in body imaging with a minimal increase in imaging time. For renal tumours in adults it is not yet possible to confidently distinguish between benign and malignant renal disease on the basis of quantitative assessment of ADC measurements alone because of considerable overlap between ADC values of benign and malignant disease [41, 42]. However, DWI can help differentiate between viable and necrotic areas within tumours that can be very useful in selecting optimal biopsy sites and detecting viable tumour after treatment [41]. Abdominal DWI is feasible in children as well. Humphries et al. [43] examined three children with nephroblastoma with DW techniques on clinical 1.5-T MR units. They confirm that DWI in children can help in guiding biopsy away from necrotic areas and suggesting poor response to chemotherapy before tumour shrinkage is expected. However, DWI was unable to differentiate between benign and malignant lesions based on ADC values alone [43].
Conclusion
For WT, a renal malignancy with an excellent prognosis, the imaging guidelines for the European therapeutic approach are outlined in the SIOP 2001 protocol. Soon this trial will be closed and the results will be evaluated. In the meantime a multidisciplinary team of physicians involved in the management of children with WT is encouraged to reflect on strategies for a new protocol in order to answer remaining questions and assist in a new risk-based approach. There is unquestionably a distinct task for radiologists who are involved in national and international paediatric oncology study groups. They will have to face several challenges including selecting the most accurate techniques (preferably non-ionizing and noninvasive) and choosing the right timing to perform them so that the minority of children who might benefit from different or more intensive therapy can be established reliably and cost-effectively.
Hopefully, the results of the SIOP 2001 trial will bring some clarity about the value of chest CT in the detection of pulmonary metastases. The future will tell if quantitative MRI techniques and/or FDG-PET will appear helpful in discriminating renal lesions and facilitate the management of bilateral disease.
For other less common childhood malignant renal tumours such as clear cell sarcoma, for which a structured diagnostic work-up is lacking, there is a need for evidence-based strategies for staging and follow-up.
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The author thanks Eline Deurloo and Koen Smets for helping with manuscript preparation.
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Smets, A.M., de Kraker, J. Malignant tumours of the kidney: imaging strategy. Pediatr Radiol 40, 1010–1018 (2010). https://doi.org/10.1007/s00247-010-1584-z
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DOI: https://doi.org/10.1007/s00247-010-1584-z