Common Uroradiological Referrals: Haematuria, Loin Pain, Renal Failure and Infection

Renal Tract Calcifications

Uroradiological referral for patients with haematuria due to stone disease is common. Approximately 95% of patients with acute renal colic have haematuria. Pathological calcification can occur in the renal parenchyma or collecting system. Nephrocalcinosis refers to the presence of calcification in the renal parenchyma; 95% of cases of nephrocalcinosis occur in the medulla and the remainder in the cortex. Medullary nephrocalcinosis is caused by hyperparathyroidism, medullary sponge kidney, renal tubular acidosis, hypervitaminosis D and primary hyperoxaluria. Cortical nephrocalcinosis is caused by acute cortical necrosis, chronic glomerulonephritis and primary hyperoxaluria. Nephrocalcinosis can be seen on conventional radiography and ultrasound (US). Stippled patterns of calcification are observed on conventional radiographs in the cortical and medullary regions of the kidneys due to cortical and medullary nephrocalcinosis, respectively. On US, increased echogenicity rather than discrete calcification may be perceived.

Nephrolithiasis refers to stone disease (calculi) in the renal collecting system. The prevalence of nephrolithiasis in patients with microscopic and macroscopic haematuria is 7.8% and 8.8%, respectively. Calcium phosphate and calcium oxalate stones, which account for most renal stones, are radio-opaque, as are struvite stones, which represent 15% of renal stones, and develop in the setting of infection and alkaline urine. Urate and xanthine stones represent 5% of renal stones and are radiolucent. Most renal stones are hyperattenuating on unenhanced computed tomography (CT) (150–1000 HU). Indinavir stones are an exception; these are associated with use of protease inhibitors and are usually radiolucent. Calcification within tumours, haematoma or fungal masses tends to have an attenuation of less than 50 HU.

Imaging of Renal and Ureteric Stones

Unenhanced CT or stone protocol CT is currently established as the one-stop imaging study of choice for renal and ureteric stone evaluation. Conventional radiography has a sensitivity of only 60% for renal stone detection, whereas US has a sensitivity and specificity for urolithiasis of 40% and 84%, respectively, compared with CT, which has a sensitivity and specificity of 98% and 97%, respectively. US tends to overestimate stone size and has reduced sensitivity and specificity for small stones and those located in the ureters. Meta-analysis of unenhanced CT compared with intravenous urography (IVU) also confirms superiority of CT for acute urolithiasis. CT radiation dose-reduction techniques have dramatically reduced dose and strengthens the case in favour of CT as first-line imaging for urolithiasis. For example, adaptive statistical iterative reconstruction blended with filtered back projection can provide diagnostic imaging at approximately 20% of the normal radiation dose ( Fig. 26.1 ). This is possible since most renal stones are conspicuous relative to surrounding tissues and therefore less radiation dose is required for diagnosis since a greater degree of image noise may be tolerated. This of course comes at the cost of potentially missing some soft-tissue attenuation lesions. CT is not only excellent for stone detection but also helps clinical decision-making. The presence and severity of ureteric or renal obstruction can be estimated and the likelihood of spontaneous stone passage may also be determined ( Fig. 26.2 ). Spontaneous passage occurs in 76% of calculi that measure 2–4 mm, 60% for calculi that measure 5–7 mm, 48% for calculi that measure 7–9 mm and less than 25% for stones greater than 9 mm.

Imaging of Renal and Ureteric Tumours

CT is excellent for the detection and assessment of renal and urothelial tumours and is considered the imaging technique of choice for renal mass evaluation. CT in this context is typically performed in the control, corticomedullary and nephrographic phases after intravenous contrast medium administration ( Fig. 26.3 ). Unenhanced CT is useful for detection of calcification in renal tumours or fat in an angiomyolipoma ( Fig. 26.4 ). Corticomedullary phase imaging is useful for cortical assessment, detection of angiogenesis in clear cell carcinoma, and recognition of pseudotumours, which may not be appreciated on later-phase imaging. Most renal and urothelial tumours are maximally conspicuous during the nephrographic phase. A difference of greater than 20 HU between unenhanced and nephrographic phase images is strongly predictive of enhancement and therefore renal neoplasm, as is a Hounsfield unit difference of greater than 10 between the corticomedullary and nephrographic phases ( Fig. 26.5 ). A difference of 10 HU between unenhanced and nephrographic phase CT is not indicative of enhancement, and a difference of 10–20 HU is equivocal. Increased attenuation can be observed in non-enhancing tissues after contrast administration due to a phenomenon known as pseudoenhancement, which is likely due to CT reconstruction algorithms. In addition, care must be taken when measuring enhancement, ensuring that the enhancing solid portion of a lesion is studied and not the cystic component ( Fig. 26.6 ). The authors have a low threshold for biopsy when imaging is equivocal as surgical management will be determined by the findings.

Radiological differentiation of benign oncocytoma from renal cell carcinoma is an ongoing challenge; oncocytomas can have a very similar appearance to renal cell carcinoma on CT ( Figs 26.7 and 26.8 ). Recent advances in magnetic resonance imaging (MRI) have provided a number of potential imaging sequences which may assist in this differentiation. A study of 48 cases demonstrated that combined differences in apparent diffusion coefficient (ADC) values and enhancement ratios provided high sensitivity and specificity for diagnosis oncocytoma over malignancy. Enhancement patterns on multiphasic MRI relative to the aorta are further potential imaging biomarkers that may aid differentiation. Although research has suggested potential solutions for this imaging challenge, these have not yet been sufficiently validated for integration into routine practice.

The high-contrast resolution of MRI is also very useful for renal lesion characterisation, especially for detection of fat within an angiomyolipoma ( Fig. 26.9 ), and diffusion- and perfusion-weighted imaging have also improved lesion detection and characterisation. CT assessment of haematuria can be performed using unenhanced CT and postintravenous contrast medium–enhanced CT, including CT urography (CTU). CTU entails imaging the kidneys and collecting systems in the pyelographic phase. Normally, the collecting systems can also be examined in the control and nephrographic phases as part of a complete CTU protocol. The CTU technique is discussed in detail in Chapter 31 . There is good evidence to indicate that traditional methods of haematuria assessment using IVU and US are improved upon by CTU. One compelling study compared retrograde ureteropyelography (UP), the imaging ‘gold standard’ for assessing the ureters and renal pelvis, with CTU. A cohort of 106 patients who had initial assessment with IVU and cystoscopy underwent CTU and UP with a 3- to 5-year follow-up period and histological reference standard. The sensitivity, specificity, positive predictive value and negative predictive value of CTU for diagnosing transitional cell carcinoma of the upper urinary tract were 0.97, 0.93, 0.79 and 0.99, respectively. This was comparable to UP. Of note, the positive predictive value of CTU, 0.79, is not very strong. Patients should have histological confirmation before undergoing surgery for findings on CTU. Urothelial cell cancers are usually visible during the nephrographic/urothelial phase of CTU, owing to the enhancement of the abnormal soft-tissue mass contrasted against the low-attenuation urine in the adjacent renal collecting system, ureter or bladder. Studies have demonstrated equivalent or higher sensitivity/specificity of nephrographic/urothelial phase CT (60 seconds) in the detection of both upper and lower tract urothelial cancers compared with excretory phase CT (5 minutes).

Imaging Features of Urothelial Tumours on Computed Tomography

Although CT has superseded IVU and US for detection of urothelial cancers, many of the imaging signs sought on CT have been previously described using IVU. Early urothelial neoplasms appear as subtle filling defects or focal mural thickening on IVU and CT. Transitional cell cancers (TCCs) can appear as fixed smooth or irregular, single or multiple filling defects within the renal collecting systems. Renal TCC can obstruct an infundibulum, creating a phantom calyx that may or may not fill with contrast. Renal TCC may also present as a central mass on US with loss of renal sinus fat echogenicity and corresponding mass on CT ( Fig. 26.10 ). Pelviureteric junction obstruction can produce a delayed nephrogram; ureteric involvement can cause acute hydronephrosis. Signs of ureteric TCC include absent renal function, eccentric or circumferential fixed wall thickening, filling defects, hydronephrosis with or without hydroureter and irregular ureteric narrowing with proximal shouldering termed the goblet sign ( Figs 26.11 and 26.12 ). Filling detects may also be produced by metastases, calculi, blood clots, infection, a vascular impression or congenital abnormality such as pyelourethritis cystica. The ultrasonic characteristics of urothelial tumours are variable. TCC is often slightly hyperechoic but may be difficult to differentiate from renal sinus fat, and further imaging is always needed for confirmation.

There are many other benign causes of haematuria which can be associated with the development of malignancy. Many causes of haematuria are diagnosed early in life using US, based on family history, or clinical findings, such as von Hippel–Lindau syndrome, tuberous sclerosis, polycystic kidney disease and medullary sponge kidney. Repeated imaging plays an essential role in screening for renal tumour development in many of these cases. MRI should be used for such screening wherever possible since contrast resolution will be superior to unenhanced CT in patients with renal insufficiency. Furthermore, even in the absence of renal insufficiency, the use of MRI will limit the number of CT studies performed over a patient's lifetime and, thereby, lifetime cumulative radiation exposure ( Fig. 26.13 ).

Haematuria as a result of trauma requires imaging to determine whether there is renal parenchymal injury, involvement of perirenal or periureteric tissues, bladder rupture and/or presence of pseudoaneurysm. Unenhanced imaging as part of CT evaluation in the setting of suspected trauma is essential. When performing angiography in the setting of iatrogenic haematuria following percutaneous nephrostomy drain insertion, an angiographic run may need to be performed while the nephrostomy drain is removed over a guidewire (which can be rapidly replaced for tamponade if required), to detect active bleeding or pseudoaneurysm formation, when not seen on initial angiographic sequences ( Fig. 26.14 ).

Imaging of Patients With Loin Pain

An ideal imaging investigation for patients with acute flank pain should be a single imaging test that provides accurate information not only about the presence or absence of urinary tract stones but also about the size and position of the calculus and the presence of related complications, such as obstruction. One of the major clinical challenges managing patients with urinary tract calculi is that symptoms are frequently non-specific and also that urinary tract calculi tend to be recurrent. In addition, there are many other potential causes of acute loin pain. Other urological causes of loin pain include blood clots or tumour in the collecting systems, obstruction of the pelviureteric junction and infection such as acute pyelonephritis (APN) or pyonephrosis. There are several non-urological causes of acute loin pain, including gall bladder problems (such as biliary colic or acute cholecystitis), abdominal aortic aneurysm leakage, pneumonia, myocardial infarction, ovarian or testicular torsion, ectopic pregnancy, appendicitis, omental infarction, epiploic appendagitis, inflammatory bowel disease, acute diverticulitis and even intervertebral disc prolapse. Chronic loin pain can be caused by urological neoplasms, including renal cell carcinoma, transitional cell carcinoma, renal and ureteric stones, tuberculosis (TB), pelviureteric junction obstruction, testicular cancer, gastrointestinal neoplasms and spinal disease. Therefore evaluation with imaging is recommended at initial presentation. This is discussed in subsequent sections. Magnetic resonance (MR) urography is still in evolution in this diagnostic setting because limited sensitivity for calcific structures remains a major limitation and, at present, MR is usually reserved for specific clinical setting (e.g. pregnant patients or following initial CT).

Useful Signs on Unenhanced Computed Tomography and Potential Pitfalls

The most important imaging finding on CT in acute ureteral obstruction secondary to urinary stone disease is direct visualisation of a calculus within the ureteric lumen. The certainty of diagnosis is strengthened by finding a dilated ureter above the stone. Definitive characterisation of a calcification as a calculus is supported by the identification of a soft-tissue rim sign . This is the detection of soft-tissue attenuation surrounding the calcification and indicates that the calcification lies within the ureter. Pelvic phleboliths do not have surrounding soft tissue, and therefore this sign is crucial for distinction. The presence of increased perinephric or periureteric fat stranding also represents a secondary sign suggestive of downstream ureteric obstruction.

There are several potential pitfalls when using unenhanced CT in the detection of urinary tract calculi and in the characterisation of an abdominal or pelvic calcification as outside the urinary tract. Calcifications of iliac vessels and their branches can be difficult to differentiate from an adjacent ureteric calculus. When it is difficult to definitively conclude that an abdominal or pelvic calcification lies within the lumen of the ureter, intravenous contrast medium administration and pyelographic phase CT can help to make the distinction between ureteric calculi and extraluminal calcifications. Currently, this strategy carries a disadvantage of increased exposure to ionising radiation and potential nephrotoxicity from iodinated contrast media. Other challenges for radiologists interpreting unenhanced CT include parapelvic cysts or an extrarenal pelvis which can mimic hydronephrosis; the distinction of these entities can be made by US or on pyelographic phase–enhanced CT. A large adnexal cyst can simulate a distended bladder. Following the entire ureteric course on unenhanced CT in a thin patient with paucity of peritoneal and retroperitoneal fat can be very difficult, and this situation can be exacerbated by the presence of multiple phleboliths in the pelvis.

Magnetic Resonance Urography

MR urography in the evaluation of patients with acute flank pain is limited by limited availability at many centres, increased study duration compared with unenhanced CT and, most importantly, substantially reduced sensitivity for urinary tract stones and therefore for definitive direct stone identification. Differentiation of a urinary stone from other intraluminal filling defects such as blood clot or tumour is difficult on MR urography. MR urography is frequently used in pregnant patients with loin pain and suspected obstructing urinary tract calculi following US of the kidneys ( Fig. 26.15 ). MR urography in this setting is useful for confirming the presence of true hydronephrosis and determining the level of apparent obstruction. As with MR urography in the non-pregnant patient, definitive detection of renal and ureteric calculi is difficult because of the limited sensitivity for calcification. Recent advances in low-dose CT have shown good sensitivity and specificity for stone diagnosis in pregnant patients, but the use of low-dose CT in this setting remains unproven and still very controversial.

Summary Box

• Macroscopic haematuria is a strong predictor of serious underlying urological pathology

• Risk factors used to triage patients with haematuria to computed tomography (CT) include age older than 40 years and macroscopic haematuria

• Unenhanced CT has excellent sensitivity and specificity for renal tract stone detection

• Renal mass protocol CT includes an unenhanced scan and corticomedullary and nephrographic phase–enhanced images

• CT urography includes a pyelographic or excretory phase scan and is currently the first-line imaging technique for suspected upper tract urothelial cancer

Chronic Renal Failure

Chronic kidney disease is divided into five stages:

• Stage 1: normal (glomerular filtration rate >90 mL/min/1.73 m ² ).

• Stage 2: mild impairment (glomerular filtration rate 60–89 mL/min/1.73 m ² ).

• Stage 3: moderate (glomerular filtration rate 31–59 mL/min/1.73 m ² ).

• Stages 4 and 5: severe (glomerular filtration rate 15–29 and < 15 mL/min/1.73 m ² , respectively).

In non-obstructive chronic renal failure, US demonstrates small kidneys with diffuse or focally reduced parenchymal thickness. As in acute renal failure, parenchymal reflectivity may be normal or increased, and increased reflectivity does not point towards a specific diagnosis. Although an increased RI may be detected in the intrarenal arteries on Doppler interrogation, this is often insufficient alone to identify the cause of renal failure. US elastography for renal assessment is currently being investigated as a means of quantifying renal fibrosis. The most common cause of chronic kidney disease is diabetes. Non-diabetic causes are divided into glomerular, vascular, tubulointerstitial and cystic aetiologies. Notable causes of renal failure relevant to imaging include the following conditions.