Abstract
Background
Focal lesions of the kidney comprise a spectrum of entities that can be broadly classified as malignant tumors, benign tumors, and non-neoplastic lesions. Malignant tumors include renal cell carcinoma subtypes, urothelial carcinoma, lymphoma, post-transplant lymphoproliferative disease, metastases to the kidney, and rare malignant lesions. Benign tumors include angiomyolipoma (fat-rich and fat-poor) and oncocytoma. Non-neoplastic lesions include infective, inflammatory, and vascular entities. Anatomical variants can also mimic focal masses.
Main body of the abstract
A range of imaging modalities are available to facilitate characterization; ultrasound (US), contrast-enhanced ultrasound (CEUS), computed tomography (CT), magnetic resonance (MR) imaging, and positron emission tomography (PET), each with their own strengths and limitations. Renal lesions are being detected with increasing frequency due to escalating imaging volumes. Accurate diagnosis is central to guiding clinical management and determining prognosis. Certain lesions require intervention, whereas others may be managed conservatively or deemed clinically insignificant. Challenging cases often benefit from a multimodality imaging approach combining the morphology, enhancement and metabolic features.
Short conclusion
Knowledge of the relevant clinical details and key imaging features is crucial for accurate characterization and differentiation of renal lesions.
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Background
Focal lesions of the kidney, broadly classified as malignant tumors, benign tumors, and non-neoplastic lesions, are being detected with increasing frequency due to escalating imaging volumes. It is incumbent upon radiologists to be familiar with the imaging appearances of these lesions and the appropriate differential diagnoses. Accurate characterization is integral to guiding clinical management and determining prognosis. Some lesions require surgery, whereas others may be managed without intervention and followed up on imaging or classified as clinically insignificant. Utilizing a multimodality imaging approach, ultrasound (US), contrast-enhanced ultrasound (CEUS), computed tomography (CT), magnetic resonance (MR) imaging, and positron emission tomography (PET), renal lesions can be characterized on the basis of morphology, enhancement, and metabolic features. In this article, we review focal renal lesions in terms of characteristic imaging features that facilitate a confident diagnosis and highlight potential pitfalls that may lead to diagnostic errors.
Malignant tumors
Renal cell carcinoma
Renal cell carcinoma (RCC) is the most common adult epithelial cancer representing 90% of renal tumors [1]. RCC accounts for 4% of all new cancer cases and its incidence is increasing by 1–2% per annum. This is attributed to an increase in the volume of imaging studies performed [2, 3]. RCC has a median age at diagnosis of 64 years and a male predilection. Several genetic conditions are associated with the development of RCCs, with von Hippel-Lindau disease the most prevalent. Environmental risk factors include smoking and obesity. RCC is classically described as presenting with the triad of flank pain, hematuria, and a flank mass; however, this only occurs in 5–10% of cases [2, 4]. A substantial proportion of RCCs are discovered incidentally [5].
The World Health Organization (WHO) classification of tumors of the kidney describes multiple subtypes or RCC [6]. RCC has three main histological subtypes; clear cell, papillary, and chromophobe. Rare RCC subtypes include collecting duct and medullary carcinomas which comprise < 1% of all renal tumors. The subtypes have separate cytogenetic and immunohistochemical profiles with varying prognosis and response to treatment. Characterizing the RCC subtype on imaging has implications for clinical management [1, 6, 7].
RCC is typically staged using the TMN system (Tables 1 and 2) [8].
Clear cell RCC
Clear cell tumor is the most common subtype accounting for 70% of RCCs [5]. This subtype has the greatest propensity to metastasize and the poorest prognosis with a 5-year survival of 44–69% [5]. At gross pathology, clear cell RCC has a characteristic golden yellow color due to an abundance of lipid-rich cells [1].
Papillary RCC
Papillary tumors account for 10–15% of RCCs [5]. They are multifocal in 23% of cases and have a lower incidence of metastases and a more favorable prognosis with a 5-year survival of 82–92% [9]. Papillary RCCs are pathologically divided into two groups; type 1 tumors have a single layer of small cells with a scanty cytoplasm and tend to have a lower Fuhrman grade. Type 2 tumors have large eosinophilic cells with pleomorphic nuclei and have a higher Fuhrman grade and a poorer prognosis [7].
Chromophobe RCC
Chromophobe tumors comprise 5% of RCCs. They also have a more favorable outcome with a 5-year survival of 78–92% [9]. Macroscopically, they are solid well-circumscribed tumors with a light brown color. Histological characteristics include large polygonal cells with prominent cell membranes [9].
Imaging of RCC
The imaging features of RCC encompass a wide spectrum from small indolent lesions to large infiltrative masses with distant spread. Several overlapping features occur with a varying frequency between subtypes including intralesional calcification, intralesional microscopic fat, bilaterality, and multifocality [9]. However, certain imaging features can assist in subtyping the lesions.
Clear cell RCCs often have a heterogeneous appearance on imaging due to necrotic, hemorrhagic, and cystic contents (Fig. 1). Doppler ultrasound shows internal vascularity while the solid component of the RCC is hypervascular on CT and MRI in the corticomedullary phase. In the nephrographic phase, the tumor demonstrates wash out, enhancing less than the adjacent renal parenchyma [10]. A large mass, retroperitoneal vascular collaterals, and renal vein thrombus (Fig. 2) suggest a high-grade tumor [7]. On MRI, clear cell RCCs demonstrate low T1 signal intensity, heterogeneous high T2 signal intensity, and are hypervascular on the corticomedullary phase. Intralesional microscopic fat may be demonstrated on chemical shift T1-weighted imaging in 60% of clear cell RCCs [7]. The presence of macroscopic fat is very rare and tends only to occur with areas of calcification (Fig. 3) [11].
Papillary RCCs are typically small (< 3 cm) peripheral lesions that are well circumscribed and homogenous. They are usually hypovascular relative to normal renal parenchyma on the corticomedullary phase of contrast-enhanced CT or MRI (Fig. 4) [5, 7]. Multi-phase CT can frequently demonstrate indeterminate enhancement (an increase of attenuation between 10 and 20 HU); further assessment with MRI or contrast-enhanced ultrasound (CEUS) is required in such instances [12]. CEUS uses gas microbubbles as a contrast medium and can demonstrate enhancement in lesions which were equivocal on CT [13].
Larger tumors (> 4 cm) can have a heterogeneous appearance due to necrosis, hemorrhage, or calcification (Fig. 5). This subtype is the most likely to be bilateral and/or multifocal. A key imaging characteristic of papillary RCC on MRI is that the tumor shows low T2 signal intensity. This MRI feature is not specific as it can also be seen in fat poor angiomyolipoma (AML). Papillary RCCs rarely contain fat. They can demonstrate areas of signal loss on in phase T1 images relative to out of phase T1 images due to hemosiderin content. The cystic variety can display papillary projections with internal blood products [7].
Chromophobe RCCs often appear as large, well-circumscribed homogeneous lesions [5]. Perinephric and vascular infiltration are rare. Contrast-enhanced CT and MR display relatively uniform enhancement in chromophobe RCCs although, in 30–40% of cases, a central stellate scar and spoke-wheel enhancement may be visualized (Fig. 6) [7, 14]. This appearance has also been reported in oncocytoma [9].
The role of PET-CT in primary RCC evaluation is limited as physiological tracer excretion by the kidney can mask the tumor. PET-CT has a more established role in re-staging advanced or recurrent RCC [9]. An emerging technique in nuclear medicine is single-photon emission computed tomography-CT (SPECT-CT) using indium-111-labelled-girentuximab. This isotope tracer recognises carbonic anhydrase IX, a specific antibody occurring in 94% of clear cell RCCs [15].
The principal differential diagnoses include AML, urothelial carcinoma (UC), oncocytoma, and lymphoma. Biopsy should be considered in instances where imaging findings are indeterminate. A biopsy can also confirm diagnosis prior to ablation and determine tumor histological grade and assist in prognostic assessment [16].
Pelvicalyceal urothelial carcinoma
Upper urinary tract UC comprises 5–10% of all urothelial tumors. Specifically, UC of the renal pelvis is estimated to represent around 15% of all renal tumors. Concurrent bladder UC occurs in 17% of cases of upper tract UC. Most upper tract UCs are superficial low-grade tumors with around 15% demonstrating infiltrative behavior [17]. Aggressive tumors can invade into the renal parenchyma without distorting the contour of the kidney. UC tends not to invade the renal veins or inferior vena cava. The incidence of upper tract UC peaks in the 7th decade and is three times more common in males than females. The principal risk factor is smoking. Upper tract UC often presents with hematuria or flank pain [18, 19].
Traditionally, excretory urography was used to detect upper tract UCs. Typical findings include a pelvicalyceal filling defect and a distended or amputated calyx due to an obstructing tumor in the infundibulum. An obstructing tumor at the ureteropelvic junction may result in hydronephrosis and poor contrast excretion. The upper tract can also be assessed during cystoscopy by a retrograde pyelogram. The imaging findings are similar to excretory urography but this technique has the advantage of facilitating cytological sampling [18, 19]. Ultrasound has limited sensitivity in detecting upper tract lesions. UC within the renal pelvis usually appears as a soft tissue mass within the echo bright renal sinus, with or without hydronephrosis. A tumor within the infundibulum may cause focal calyceal dilatation. Infiltrative UC may extend into the renal cortex where it typically appears slightly hyperechoic compared with the adjacent renal parenchyma [18, 19].
CT urography is the technique of choice. On the excretory phase, pelvicalyceal UC typically appears as a sessile filling defect, a mass lesion, or circumferential wall thickening (Fig. 7). The nephrographic phase can complement the excretory phase, demonstrating the tumor as an enhancing soft-tissue mass against the background of the lower attenuation collecting system [20, 21]. Rarely, UC may contain tiny calcifications. An aggressive UC obliterating the sinus fat and infiltrating into the renal parenchyma may be seen as a hypoenhancing mass distorting the renal architecture with a resultant delayed nephrogram. This type of lesion is actually most reliably visualized on the corticomedullary phase. A large infiltrating pelvicalyceal UC can be difficult to differentiate from an RCC. Preservation of the reniform shape favors UC over RCC. Areas of necrosis may be seen in infiltrating UCs and it can be challenging to differentiate such a lesion from RCC, lymphoma, or xanthogranulomatous pyelonephritis (XGP) [21]. MR urography can be performed without intravenous contrast and may be helpful in evaluating UC in cases where contrast agents are contraindicated. Pre-contrast T1 sequences can be useful in excluding hemorrhage as a cause of a urothelial filling defect. Diffusion-weighted imaging (DWI) and apparent diffusion coefficient (ADC) maps have been shown to be useful in staging and predicting the histological grade of the tumor [22, 23]. Similar to RCC, the role of FDG PET-CT in upper tract UC diagnosis is limited as physiological tracer excretion by the kidney can mask the tumor. PET-CT can be used in staging advanced or recurrent UC [17].
Upper tract UC is typically staged using the TMN system (Tables 3 and 4) [24].
Lymphoma
Most cases of renal lymphoma occur as part of extensive disease affecting multiple solid organs or retroperitoneal nodes and is classified as secondary lymphoma. The histology is typically B cell non-Hodgkin’s lymphoma (NHL). Primary renal lymphoma accounts for < 1% of extranodal NHL [25, 26]. It is classified as isolated renal disease without associated mediastinal or pelvic adenopathy. Primary renal lymphoma occurs most frequently in middle-aged men and often presents with flank pain, weight loss, or fatigue [26].
Secondary renal lymphoma can present as single or multiple focal lesions in one or both kidneys. It may also arise in the perinephric region, the renal sinus, or cause nephromegaly.
The most common imaging manifestation of primary renal lymphoma is that of multiple renal masses, accounting for 40–60% of cases. Less common findings include direct extension to the kidneys from retroperitoneal adenopathy, diffuse renal involvement where the kidneys are enlarged but maintain their reniform shape, and a perinephric mass. In both types of renal lymphoma, the lesions are typically hypovascular—this feature may assist in differentiating lymphoma from other neoplasms that typically show greater enhancement. Renal lymphoma is usually a solid lesion that is hypoechoic relative to the renal parenchyma on ultrasound. CT typically demonstrates a homogenous lesion that shows minimal enhancement. The lesions may infiltrate the renal parenchyma or sinus with preservation of the reniform shape. A characteristic finding is the renal veins and arteries usually remain patent despite encasement. Retroperitoneal lymphadenopathy is common. Associated findings may include splenomegaly. On MRI, lymphomatous lesions are usually hypointense on T2-weighted images and iso- to mildly hypointense on T1-weighted images relative to the normal cortex (Fig. 8). Following contrast administration, the lesions enhance to a lesser degree than the adjacent normal cortex [25, 27]. The lesions show avid uptake of FDG on PET and have been shown to have a higher standardised uptake value compared to RCCs [28]. The main differential diagnoses include RCC, upper tract UC, and focal pyelonephritis. Percutaneous biopsy is typically required for diagnosis due to non-specific imaging findings [26].
Post-transplant lymphoproliferative disease
Post-transplant lymphoproliferative disease (PTLD) refers to a collection of lymphoproliferative diseases that develop after solid organ or stem cell transplantation [25, 29]. The disease spectrum ranges from abnormal lymphoid hyperplasia to frank malignancy. The majority of cases of PTLD are associated with proliferation of B lymphocytes due to Epstein-Barr virus infection. The incidence of PTLD ranges from 1 to 20% and is dependent on the transplanted organ. It develops in up to 20% of small bowel transplant recipients, 1–11% of heart transplant recipients, 2–10% of lung transplant recipients, 1–3% of renal transplant recipients, and 1–3% of liver transplant recipients [30]. PTLD occurs most frequently in the first 12 months following transplantation and is more common in pediatric patients. PTLD can occur in any anatomical location but it is most common within the abdomen and is extranodal in 80%. The three most common sites in the abdomen are the liver (50%), small bowel (25%), and kidneys (17%) [26]. In renal transplant recipients, the allograft is the most frequently affected organ. PTLD can also occur in the native kidneys following transplantation of other organs. Treatment strategies include lowering the dose of immunosuppression, chemoradiation, or antiviral therapy. Despite treatment, the mortality is 30–60% [29].
Typical CT imaging findings in renal allograft PTLD include a heterogeneous hilar mass that may encase vessels or multiple hypovascular parenchymal lesions (Fig. 9). On MRI, these focal lesions are iso- to hypointense relative to the renal parenchyma on T1-weighted images and mildly hypointense on T2-weighted images. PTLD lesions tend to be FDG avid on PET. Diffuse infiltrative disease with nephromegaly has been described [25, 30]. PTLD should be considered in any new visceral lesion or lymphadenopathy in a transplant patient [29]. A biopsy may be required to confirm the diagnosis. The differential diagnoses include a new or recurrent malignancy and focal pyelonephritis.
Metastases to the Kidney
Isolated metastases to the kidney are rare. Typically, metastatic involvement of the kidneys occurs in diffuse dissemination of the primary malignancy. In these cases, the renal lesions tend to be multiple and bilateral. The most common primaries include the lungs followed by the breast, gastrointestinal tract, and melanoma [31, 32]. Studies have reported a wide range of time intervals between diagnosis of the primary tumor and detection of the renal metastases. One of the largest recent studies by Wu et al. reported a median interval of 3.1 years with a range of < 1 year to > 20 years [31]. Overall, it is difficult to establish patient prognosis from the limited number of small studies available [32, 33].
Metastases to the kidney tend to be encountered incidentally on imaging. Despite the absence of pathognomonic imaging features, there are several clues that suggest the diagnosis [33, 34]. Firstly, this involves being aware that there is a background history of cancer. The study by Wu at al. reported that in 88% of cases, there was a known history of primary cancer [31]. Secondly, metastases are typically hypovascular and endophytic on CT/MRI (Fig. 10) [34]. However, due to the low incidence of renal metastases and overlapping imaging features with other lesions such as RCC, a biopsy may ultimately be required [31].
Benign tumors
Angiomyolipoma
AML is the most frequently encountered solid benign renal tumor and is classified as a perivascular epithelioid cell tumor. AMLs contain variable amounts of dysmorphic blood vessels, smooth muscle cells, and adipose tissue. Recent recognition that renal AMLs comprise a heterogeneous group of lesions with a spectrum of pathological and radiological characteristics has led to the creation of a classification system by Jinzaki et al [11, 35]. The majority of renal AMLs occur sporadically. The remainder of AMLs is associated with syndromes such as tuberous sclerosis and lymphangioleiomyomatosis [36].
Based on imaging characteristics, benign AMLs can be split into classic (fat-rich) and fat-poor. The fat-poor AMLs can be subdivided into hyperattenuating AML, isoattenuating AML, and angiomyolipoma with epithelial cysts (AMLEC) [11]. Benign AMLs have an incidence rate of < 0.2% and occur most commonly in middle-aged females [34]. They tend to be discovered incidentally but can present with spontaneous hemorrhage particularly if ≥ 4 cm [37].
Classic AMLs are by far the most common subtype. Internal macroscopic fat is their characteristic feature. On ultrasound, they typically appear uniformly hyperechoic compared to normal renal parenchyma (Fig. 11). However, occasionally, an RCC can also appear uniformly hyperechoic and mimic an AML. Hypoattenuating regions (< – 10 HU) on unenhanced CT suggests macroscopic fat within an AML. Hemorrhage within an AML can mask the fat content. Contrast-enhanced CT is not usually required to diagnose a classic AML but is useful to demonstrate the vascular anatomy prior to embolization of large lesions. Macroscopic fat will appear hyperintense relative to the renal parenchyma on T1- and T2-weighted MR sequences and show signal loss on fat-suppressed sequences. In and out of phase imaging creates an India ink artifact at the interface between fat and soft tissue or fluid. This interface will appear at the border between the AML and renal parenchyma or within the lesion between fat and non-fatty components. Internal signal loss on opposed-phase T1 images compared to in-phase T1 images indicates the presence of microscopic fat—this may be seen in both AMLs and RCCs. The main differential diagnosis for a classic AML includes retroperitoneal liposarcoma and RCC. An exophytic AML will typically demonstrate a small defect in the renal cortex (“claw” sign) and a feeding vessel to the underlying kidney—this allows differentiation from a liposarcoma rarely contain fat cells originating in the kidney. Classic AMLs are differentiated from RCCs by macroscopic fat. Although RCCs can rarely contain macroscopic fat, it is often associated with calcifications [11, 35].
Hyperattenuating AMLs are a fat-poor subtype and comprises 5% of all AMLs. On ultrasound, it is generally uniformly isoechoic relative to muscle. On unenhanced CT, these lesions are usually small and hyperattenuating compared to renal parenchyma. They tend to enhance homogenously and avidly on CT and MRI. Hyperattenuating AMLs are hypointense on T1- and T2-weighted sequences and they generally do not demonstrate any signal loss on fat-suppressed and out of phase T1-weighted sequences. Both fat-poor AMLs and papillary RCCs show low T2 signal intensity. If the lesion enhances homogeneously, then a hyperattenuating AML should be considered (Fig. 12). A biopsy is recommended to confirm the diagnosis [11, 35].
The isoattenuating AML fat-poor subtype is rare. These lesions are of a similar attenuation to renal parenchyma on unenhanced CT. MR features include hypointensity on T2-weighted images and signal loss on out of phase T1-weighted images compared to in-phase images. This subtype cannot be reliably distinguished from clear cell RCC on imaging [11, 35].
AMLEC is the least common fat-poor subtype. It can be potentially malignant or overtly malignant. Imaging features include a hyperattenuating lesion on unenhanced CT and hypointense regions or septations with hyperintense cystic components on T2-weighted images. A biopsy is required for definitive diagnosis [11, 35].
Oncocytoma
Oncocytoma is the second most common benign tumor comprising 3–7% of renal neoplasms. It has a peak incidence in the 7th decade and a slight male predominance [38, 39]. On histopathology, oncocytoma classically demonstrates nests and tubular structures lined with eosinophilic granular cytoplasm. However, variations in these features result in considerable overlap with chromophobe RCCs [40]. Oncocytoma and chromophobe RCCs also share common findings at gross pathology and imaging. Oncocytomas are often clinically silent but can present with pain or hematuria [39, 41].
Imaging findings can be variable due to the spectrum of cellular patterns that can influence tumor enhancement. Features suggestive, but not pathognomonic, of an oncocytoma includes a solid well-defined lesion with a central stellate scar (Fig. 13) and spoke wheel enhancement as well as segmental enhancement inversion [9, 42]. This latter finding represents two different areas of intralesional enhancement on the arterial phase that displays corresponding enhancement reversal on the excretory phase on CT/MRI [43]. Rare features include calcification, hemorrhage, cystic foci, and aggressive behavior [38]. Recent studies using sestamibi single-photon emission CT to distinguish between oncocytoma and RCC have shown promising results, although further studies are required [44, 45]. As a result of the absence of pathognomonic imaging characteristics, a biopsy is often performed. However, pathological assessment of a core biopsy can be problematic as the sample may not be representative of the entire lesion [19]. In instances where the biopsy is suggestive of an oncocytoma but surgery is declined, active surveillance should be considered to avoid missing an RCC [38].
Non-neoplastic lesions
Infection
Acute bacterial pyelonephritis typically results from ascending migration of an infectious bladder organism. The diagnosis is often made clinically based on symptoms, blood tests, and urinalysis. Imaging is not required in mild cases but is crucial in cases where the diagnosis is not clear or in patients with complicating factors such as immunosuppression or where there is a failure to respond to therapy [46].
Sonographic abnormalities include focal or generalized renal enlargement, focal changes in renal parenchymal echogenicity, reduced corticomedullary differentiation, and focal areas of reduced Doppler flow. However, in early disease, the kidneys can appear normal on US. Contrast-enhanced CT is the modality of choice for detecting pyelonephritis—this may manifest as a wedge-shaped or rounded region of reduced or streaky enhancement with adjacent perinephric inflammatory change (Fig. 14) [46]. A striated nephrogram may also be seen. Occasionally, pyelonephritis can appear as a rounded lesion that displays mass effect. Such cases can be challenging to distinguish from a neoplasm.
Intraparenchymal or perinephric abscesses may develop as a complication of pyelonephritis. Abscess formation should be suspected in cases where appropriate antibiotics have not resulted in clinical improvement, particularly if the patient is immunosuppressed. Sonographic features include a fluid collection with internal debris and septations. On CT, renal abscesses are usually round areas of low attenuation with an enhancing rim and adjacent inflammatory stranding (Fig. 15). Internal gas may be present. MRI findings are similar to CT with the internal contents demonstrating fluid signal characteristics and rim enhancement following gadolinium [46, 47].
XGP is induced by chronic renal obstruction and infection resulting in parenchymal destruction and replacement with lipid-laden macrophages. The most common pathogens are Escherichia coli and Proteus mirabilis. The condition typically occurs in immunocompromised middle-aged females. Symptoms are frequently non-specific [48, 49]. Typical imaging findings across modalities include renal enlargement and a large obstructing staghorn calculus. XGP can rarely occur as a focal lesion and can be challenging to differentiate from a neoplasm. CT is the most useful modality in confirming the diagnosis and can facilitate surgical planning. Typical CT findings include a renal pelvis contracted around a staghorn calculus, caliectasis, inflammatory changes in the kidney, and fibrofatty proliferation in the surrounding tissues (Fig. 16) [49].
Immunocompromised patients are vulnerable to opportunistic infections, such as Mycobacterium and fungal infections. Renal tuberculosis (TB) causes papillary necrosis and parenchymal destruction. CT findings include caliectasis, strictures of the renal pelvis/infundibula, and calcifications [50]. Common fungal organisms include Candida and Aspergillus. On imaging, these infections can manifest as renal abscesses or hydronephrosis with filling defects in the dilated pelvicalyceal system. Microbiological tests are required to confirm the diagnosis [46, 51].
Inflammatory
Sarcoid
Sarcoidosis is a multisystem disorder characterized pathologically by the presence of non-caseating granulomas. Sarcoidosis has a female predominance and a peak incidence at 20–39 years of age. It is roughly three times more prevalent in Americans of African descent compared with Caucasian Americans. Around 90% of patients have thoracic manifestations and approximately 30% have extra-pulmonary disease [52, 53]. Renal sarcoidosis may present clinically with signs of altered calcium metabolism—this includes nephrocalcinosis, hypercalcemia, and hypercalciuria. Renal impairment can occur due to interstitial nephritis. Granulomatous involvement of the kidney can also be asymptomatic [54, 55]. Renal granulomas have been reported in 22% of sarcoid patients at autopsy but radiologically distinct granulomas are uncommon [52].
Granulomatous deposits within kidneys are often referred to as pseudotumors. These lesions can be single or multiple and have varied imaging appearances. Hypoechoic and hyperechoic lesions have both been reported on US [52, 56]. On CT, the masses may be hypo-, iso-, or hyperattenuating relative to the renal parenchyma. Following contrast administration, they may or may not demonstrate enhancement. Renal sarcoidosis causing interstitial nephritis can produce a striated nephrogram on contrast-enhanced CT. MRI depicts pseudotumors as homogenous or heterogeneous lesions that are hypovascular on postcontrast images [53, 57]. On PET imaging using 18F-fluorodeoxyglucose, the renal granulomas have been reported to demonstrate avid tracer uptake. Due to the non-specific imaging appearance of renal sarcoid, it cannot be distinguished from other infiltrative renal masses. The presence of typical features of sarcoid in the chest may place it higher in the list of differential diagnoses but biopsy is needed for definitive diagnosis [53, 57].
IgG4-related kidney disease
IgG4-related kidney disease is a relatively newly recognized condition. This autoimmune disease affects a variety of organs, the pancreas being the most common [58]. Histopathologically, it is characterized by the presence of a dense lymphoplasmacytic infiltrate with an abundance of IgG4-positive plasma cells and fibrosis [59]. IgG4-related kidney disease most frequently occurs in middle-aged or elderly patients and has a predilection for males. The condition typically occurs in conjunction with other organ involvement. In the early stages, the patient may be asymptomatic. Advanced IgG4-related kidney disease can cause renal failure secondary to tubulointerstitial nephritis followed by glomerular disease. Urinalysis may show proteinuria. Serum IgG4 levels are frequently elevated [58, 60].
IgG4-related kidney disease can arise with the renal parenchyma (round or wedge-shaped lesions), renal pelvis, or perinephric region reference [61]. Generalized renal enlargement has also been described. The renal parenchyma is the most common location and lesions can appear as single or multiple nodules or diffuse patchy infiltrative lesions. Ultrasound findings tend to be non-specific. Sonographic features include poorly defined regions of reduced echogenicity and there may be irregularity of the renal contour. CT demonstrates rounded or wedge-shaped hypoenhancing lesions [58, 60]. On MRI, the lesions show low signal on T1- and T2-weighted images and display mild enhancement. DWI sequences have been shown to be helpful in detecting subclinical lesions [61, 62]. Renal pelvis or perinephric lesions are much less common. The presence of extra-renal disease and serum IgG4 levels can help clinch the diagnosis [60].
Vascular and hemorrhagic lesions
Renal infarction
Renal infarction results from impaired arterial supply or venous drainage. Common causes include thromboembolic disease, renal artery abnormalities (dissection, aneurysm, and fibromuscular dysplasia), trauma, or vasculitis [63, 64]. Acute renal infarction can rarely present with flank pain or hematuria. It is usually detected incidentally on imaging [64].
Contrast-enhanced CT is the first-choice imaging modality for detecting renal infarction. Typical findings are one or more wedge-shaped regions of hypoattenuation (denoting non-enhancement) involving the cortex and medulla (Fig. 17). More diffuse infarcts may display mass effect. In these cases, the presence of a thin rim of cortical enhancement (cortical rim sign) adjacent to the hypoattenuating renal parenchyma is virtually pathognomonic for an infarct. A flip-flop enhancement pattern has also been described where the region of reduced attenuation demonstrates delayed enhancement on later phases. This feature can be helpful in differentiating an infarct from a tumor. It is also crucial to assess other organs for the presence of additional infarcts and the vasculature for a potential causative etiology [64, 65]. In patients with contraindications for intravenous contrast, an alternative modality is CEUS. This technique has been shown to have comparable accuracy to CT. Renal infarction appears as a wedge-shaped region of non-perfusion on CEUS [66].
Renal artery aneurysm
Renal artery aneurysms have a prevalence of 0.01–1% [67]. They are frequently saccular and are more common in females. Fibromuscular dysplasia and atherosclerosis are the most common etiological factors. Patients typically present in the sixth decade of life usually as an incidental discovery on imaging. A small proportion of patients present with symptoms due to rupture or from thromboembolic disease [68]. The majority of renal artery aneurysms arise at the main renal artery division. Around 10% occur within the renal parenchyma and can mimic solid or cystic renal lesions on imaging. Any anechoic lesion in the renal sinus should be assessed with color-Doppler to rule out an aneurysm. Ultrasound with color Doppler characteristically shows turbulent flow with communication to the renal artery. The presence of thrombus or calcification within the aneurysm may result in undetectable Doppler signal (Fig. 18). In such instances, evaluation with CT and/or MRI should provide definitive characterization [67, 69].
Benign hyperattenuating cysts
Benign cysts containing hemorrhage or proteinaceous content are responsible for the vast majority of hyperattenuating renal lesions. Key imaging features include small size (≤ 3 cm), clearly defined margins with at least one quarter abutting perinephric fat, homogenous hyperattenuation, and absence of enhancement (on CT an increase in attenuation by 10 HU following contrast). An increase in attenuation ≥ 20 HU is considered enhancement while an increase of 10–20 HU is considered indeterminate. Beam hardening and partial volume averaging on contrast-enhanced CT can present a potential pitfall through pseudoenhacement, i.e., an artificial increase in attenuation [70, 71]. The recent White Paper by the ACR on the management of the incidental renal mass on CT stated that a homogenous mass of ≥ 70 HU on unenhanced CT is almost always a hyperdense Bosniak II cyst and requires no further evaluation [70]. However, a lesion of the same attenuation detected on contrast-enhanced CT is indeterminate and should be characterized further with a multiphase CT or MRI. A heterogenous hyperattenuating lesion also requires multiphase imaging for characterization. MRI is the imaging modality of choice and can detect internal hemorrhage or proteinaceous material due to their T1 hyperintensity (Fig. 19) [70, 72]. Post gadolinium subtraction sequences are useful for differentiating a renal neoplasm with secondary intratumoral hemorrhage from a simple hemorrhagic or proteinaceous renal cyst [73]. CEUS can also be used to assess for intralesional enhancement [66].
Anatomical variants
A prominent column of Bertin is an anatomical variant that can mimic a mass. It results from hypertrophied cortical tissue. This pseudomass typically occurs between upper and interpolar calyces and is more common on the left. On contrast-enhanced CT and MRI, the enhancement pattern in a column of Bertin should be identical to the renal cortex on all phases—this is most evident on the corticomedullary phase (Fig. 20). The absence of cortical disruption allows differentiation from RCC [74, 75].
A dromedary hump is another anatomical variant that can be mistaken for a mass. It is due to the splenic impression and appears as a focal bulge on the superolateral portion of the left kidney. Similar to a prominent column of Bertin, the enhancement pattern should match that of the adjacent renal cortex on all post contrast phases (Fig. 21) [74, 76].
Small renal mass in clinical practice
Detection of an incidental small renal mass (≤ 4 cm) on imaging is a common situation for a radiologist. The lesion will either be completely characterized or it will be indeterminate. These indeterminate lesions will typically go on to have a multiphase CT or MRI unless there are benign features such as previous imaging showing stability over at least 5 years [70, 77]. Were image findings are consistent with localized RCC, there are a variety treatment options available depending on the patient profile. For instance, young patients will typically be offered a nephrectomy or nephron-sparing surgery, whereas patients with a limited life expectancy or significant comorbidity could be considered for active surveillance or percutaneous ablation [70, 78]. In cases which remain indeterminate following a multiphase CT or MRI, further workup options include percutaneous biopsy or alternative imagining techniques [77].
Renal mass biopsy
Percutaneous renal mass biopsy is a safe procedure with a high diagnostic yield. It has a crucial role in the work up of indeterminate renal lesions and assisting clinical decisions in the following scenarios; patients with a renal mass and an extra-renal malignancy to distinguish between separate primaries and a metastasis to the kidney, patients with likely metastatic/unresectable renal malignancy to allow sub typing for potential systemic therapy, patients with a small renal mass (≤ 4 cm) which may be suitable for active surveillance or minimally invasive treatments, and patients with multiple/bilateral renal masses who may have an underlying hereditary condition [77, 79].
Alternative imaging techniques
CEUS using intravenous microbubbles allows dynamic assessment of microvasculature. It can therefore assist differentiation between cystic and solid lesions and characterization of complex cystic lesions. It is a useful tool in patients who have contraindications for iodinated contrast or MRI [77].
Dual energy CT can create virtual non-contrast images from a single-phase contrast-enhanced scan. It is particularly helpful with incidental lesions detected on a single-phase post contrast CT were the virtual non-contrast images can differentiate between a soft tissue tumor and a hyper dense cyst without requiring a repeat multiphase CT [77, 80].
Tc-99m sestamibi single-photon emission computed tomography (SPECT)/CT has shown promise in a number of studies at differentiating oncocytoma and RCC, with oncocytoma demonstrating positive tracer uptake and RCC being negative [81].
Conclusion
Focal lesions of the kidney can be caused by a range of malignant tumors, benign tumors, and non-neoplastic entities. Lesions can have overlapping radiological features requiring a multimodality imaging approach. Knowledge of relevant clinical details and key imaging features is crucial for accurate characterization and differentiation.
Availability of data and materials
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Abbreviations
- AML:
-
Angiomyolipoma
- AMLEC:
-
Angiomyolipoma with epithelial cysts
- CEUS:
-
Contrast-enhanced ultrasound
- CT:
-
Computed tomography
- MRI:
-
Magnetic resonance imaging
- PET:
-
Positron emission tomography
- PTLD:
-
Post-transplant lymphoproliferative disorder
- RCC:
-
Renal cell carcinoma
- RT:
-
Renal tuberculosis
- SPECT-CT:
-
Single-photon emission computed tomography-CT
- UC:
-
Urothelial carcinoma
- US:
-
Ultrasound
- WHO:
-
World Health Organization
- XGP:
-
Xanthogranulomatous pyelonephritis
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Lyske, J., Mathew, R.P., Hutchinson, C. et al. Multimodality imaging review of focal renal lesions. Egypt J Radiol Nucl Med 52, 14 (2021). https://doi.org/10.1186/s43055-020-00391-z
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DOI: https://doi.org/10.1186/s43055-020-00391-z