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DMSA scan

A DMSA scan, also known as dimercaptosuccinic acid renal , is a imaging procedure that uses a bound to to visualize the and assess kidney structure and function. The tracer, Tc-99m DMSA, is injected intravenously and binds to proximal tubular cells in the kidneys, allowing gamma cameras to capture detailed static images of cortical tissue after an accumulation period of 90 minutes to 4 hours. This scan is particularly valued for its high in detecting renal parenchymal abnormalities without evaluating dynamic processes. The procedure typically begins with the intravenous administration of the radiotracer, dosed at approximately 5 for adults or 0.05 / for children (up to a maximum of 2.7 ), followed by using a with pinhole or low-energy collimators to produce high-resolution views of the kidneys. Patients must remain still during the 30- to 60-minute scan, which may require in young children to ensure image quality; for sedated children, guidelines such as no solid food for 8 hours or clear liquids for 2 hours apply. is encouraged before and after the procedure to facilitate tracer clearance, and the effective dose is low, around 1 mSv, which is lower than a typical chest (5-7 mSv). Contraindications include due to fetal risks, and should be paused for 4-12 hours post-scan. DMSA scans are primarily indicated for evaluating renal scarring or damage from urinary tract infections, particularly in children where they detect early with high accuracy in those over 5 years old. In both pediatric and adult populations, they assess cortical defects, congenital anomalies, renal masses (distinguishing functioning from nonfunctioning tissue), and pre-surgical function, aiding in targeted therapies like radiotherapy. Results, interpreted by specialists, are typically available within 24 hours and provide quantitative data on relative renal function, such as split function percentages between kidneys.

Overview

Definition and purpose

A DMSA scan, or dimercaptosuccinic acid scan, is a form of renal cortical in that employs labeled dimercaptosuccinic acid (99mTc-DMSA) to produce static images of the renal . This allows for detailed of the kidney's cortical by capturing the distribution of the radiotracer in the renal tissue. The primary purpose of the DMSA scan is to evaluate renal morphology, assess the of the , and quantify relative renal function between the two kidneys, without measuring dynamic aspects such as urinary or renal blood flow. Unlike dynamic scans that use agents like DTPA or MAG3 to study excretory pathways, the DMSA scan focuses on static parenchymal evaluation to identify areas of functional tissue. At the cellular level, 99mTc-DMSA binds preferentially to proximal tubular cells in the , highlighting viable cortical tissue rather than relying on glomerular mechanisms. This mechanism provides high-resolution images of functioning nephrons, making it particularly useful for detecting structural anomalies. Developed in the 1970s, 99mTc-DMSA was introduced as a safer alternative to earlier renal imaging agents such as ortho-iodohippurate, which involved higher radiation doses from isotopes like ; the label offered superior imaging properties and lower patient exposure. The seminal clinical evaluation of this agent was reported in 1975, establishing its role in routine renal .

Radiopharmaceutical agent

The agent employed in DMSA scans is dimercaptosuccinic acid (99mTc-DMSA), in which dimercaptosuccinic acid (DMSA)—a chelating with the C4H6O4S2 and known systematically as 2,3-dimercaptosuccinic acid—forms a stable with the . Under acidic conditions ( 2.5–3.5), DMSA coordinates with in the +3 via its two sulfhydryl (-SH) groups and one , yielding the hexacoordinated 99mTc(III)-DMSA complex, which is the predominant form for renal cortical imaging due to its stability and targeted binding properties. Preparation of 99mTc-DMSA utilizes a commercial freeze-dried typically containing 1–3 mg DMSA, 0.2–1 mg stannous chloride dihydrate (as a ), and an such as 3 mg ascorbic acid, reconstituted under aseptic conditions by adding 2–5 mL of sodium pertechnetate (99mTcO4-) eluate (up to 3.7 GBq or 100 ). The mixture is gently agitated and allowed to react at for 10–30 minutes, achieving >95% radiochemical purity as verified by , before sterile filtration if needed; the final product is administered intravenously as a clear at neutral . Administered activities are standardized for safety: 74–185 MBq (2–5 ) for adults, with pediatric dosing scaled by weight at approximately 1.85 MBq/kg (50 μCi/kg), equating to 0.5–1 per 10 kg body weight and a minimum of 18.5 MBq (0.5 ). The physical characteristics of 99mTc enable efficient imaging: it decays by isomeric transition with a half-life of 6.01 hours, emitting monochromatic gamma photons at 140.5 keV (89% abundance) suitable for detection by gamma cameras equipped with low-energy high-resolution collimators, while delivering an effective dose of approximately 0.6–1 mSv per 74–185 MBq administered to adults. In vivo, 99mTc-DMSA demonstrates favorable biodistribution for renal assessment, with 40–50% of the injected dose accumulating in the kidneys by 2–4 hours post-injection, predominantly via (70–90%) followed by uptake into proximal tubular cells through megalin-mediated , and exhibiting minimal urinary (<10% over 24 hours) due to its cortical retention rather than glomerular . The remaining activity clears slowly via hepatobiliary and reticuloendothelial pathways, with <5% in the liver and <2% in other organs at peak renal uptake.

Clinical indications

Renal scarring and congenital anomalies

DMSA scans are particularly valuable for detecting renal cortical scarring resulting from (VUR) or recurrent urinary tract infections (UTIs), where the radiotracer highlights areas of parenchymal damage as focal defects in cortical uptake. This imaging modality serves as the gold standard for identifying such scars, offering high sensitivity for focal defects and superior detection compared to ultrasonography alone. In the context of congenital anomalies, DMSA scans effectively characterize structural kidney defects by demonstrating differential uptake and function, including absent or small kidneys (indicating or ), ectopic kidneys (such as pelvic or cross-fused ectopia), duplex collecting systems (with split uptake patterns), and horseshoe kidneys (showing fused cortical tissue). These findings help confirm non-functional or dysplastic tissue and assess overall renal contribution. Among children with VUR, DMSA scans identify renal scars in 30-50% of cases, providing critical evidence to guide management decisions such as ureteral reimplantation for high-grade to prevent further damage. Serial DMSA scans play a key role in follow-up for patients with high-grade , allowing monitoring of scar progression or stability over time and evaluation of relative renal through split uptake percentages.

Acute infections and hypertension evaluation

DMSA scans are employed to diagnose acute in children, where focal or global cortical defects on signify areas of and impaired renal function due to active . These defects arise from reduced uptake of the radiotracer in inflamed , confirming upper urinary tract involvement when lower tract symptoms alone are inconclusive. A 2020 meta-analysis of clinical studies reported an overall sensitivity of 91% and specificity of 99% for DMSA in detecting acute . Higher thresholds for (SPECT) can enhance detection accuracy. In young patients with , DMSA scans can aid in evaluating differential renal , particularly in cases of suspected unilateral , though captopril-augmented or ACE inhibitor-enhanced protocols are preferred for assessing hemodynamically significant . Per the 2011 guidelines on febrile urinary tract infections, which remain current as of , DMSA scans are not recommended for routine initial evaluation in infants aged 2 to 24 months; renal and bladder is advised post-UTI, with for hydronephrosis, scarring, or recurrence. DMSA may be used to assess for renal parenchymal involvement in select cases of or recurrent infections. In acute infection settings, early performance of the scan—within days of symptom onset—can overestimate permanent scarring, as reversible inflammatory defects may appear similar to lesions; guidelines advise delaying follow-up imaging by 3 to 6 months to accurately differentiate acute changes from lasting damage.

Procedure

Patient preparation

Patients undergoing a DMSA scan require minimal preparation to ensure optimal tracer distribution and image quality while minimizing to non-target areas. No is necessary, and patients are encouraged to maintain good by drinking plenty of oral fluids prior to the procedure, which helps promote the distribution of the and reduces the radiation dose to the wall. There are no specific dietary restrictions, allowing patients to eat normally before the scan. Regarding medications, no routine adjustments are required, though patients should inform the medical team of any known allergies to technetium-based agents, which are exceedingly rare. The scan is typically scheduled for imaging 2 to 6 hours after intravenous injection of the DMSA tracer, allowing sufficient time for uptake in the . Patients are advised to void their immediately before imaging to facilitate accurate evaluation of the upper urinary tract and avoid artifacts from a full . In pediatric patients, who comprise a significant portion of DMSA scan recipients due to its utility in evaluating renal anomalies, preparation may include sleep deprivation for infants to promote natural sedation during the prolonged imaging session, or pharmacological sedation for young or uncooperative children if distraction techniques prove insufficient. For pregnant individuals, the procedure carries a small risk of fetal radiation exposure, so it is generally deferred unless clinically essential; women who may be pregnant must notify the healthcare team beforehand for risk-benefit assessment. Pregnant women and young children should also avoid accompanying the patient during the injection and imaging to limit extraneous radiation exposure.

Tracer administration and imaging

The radiopharmaceutical agent, ^{99m}Tc-DMSA, is administered via intravenous injection to ensure direct access to the bloodstream for renal uptake. For adults, the typical administered activity is 111 MBq (3 mCi), while pediatric dosing is weight-based (e.g., 1.85 MBq/kg with a minimum of 18.5 MBq for small infants), following the EANM Paediatric Dosage Card or North American Consensus Guidelines (as of 2024) to minimize radiation exposure. Care is taken to avoid extravasation at the injection site, which could lead to non-physiological tracer distribution and imaging artifacts. Following administration, imaging is delayed for 2-4 hours in adults or 2-3 hours in children to allow sufficient renal cortical binding of the tracer, which reaches approximately 40-50% uptake in normal kidneys during this period; longer delays up to 24 hours may be used in cases of impaired renal function. Imaging is conducted using a with a low-energy high-resolution (LEHR) or low-energy ultra-high-resolution (LEUHR) , optimized for the 140 keV emissions of ^{99m}Tc. Standard planar acquires static images in posterior, anterior, and 30°-35° posterior views, with the patient positioned to reduce motion; acquisition continues for 5-10 minutes per view or until 200,000-500,000 total counts are achieved, using a 128×128 or 256×256 matrix with 2-4 mm pixel size. In pediatric patients, particularly infants, a pinhole (3-4 mm aperture) is preferred for higher , targeting 100,000-150,000 counts or 6-8 minutes per view. For three-dimensional assessment, (SPECT) may be performed, acquiring 120 projections over 360° at 15-20 seconds per projection, often combined with low-dose for attenuation correction. Optional whole-body imaging can be included to evaluate for ectopic renal tissue. Quality control measures include verifying adequate count statistics (e.g., 300,000-500,000 counts for planar views), assessing for patient motion through cine review, and confirming no injection extravasation to ensure image quality and diagnostic accuracy.

Image interpretation

Normal findings

In a normal DMSA scan, the renal cortices exhibit symmetric and homogeneous uptake of the radiotracer, appearing as smooth, continuous, and well-delineated structures with high intensity relative to the background. This uptake is confined primarily to the cortical parenchyma, demonstrating clear corticomedullary differentiation where the cortex appears hyperintense and the central renal sinus, encompassing the pelvis and calyces, shows relative photopenia. No focal defects, indentations, or areas of reduced uptake (photopenic regions) are present, confirming intact cortical architecture and function. Anatomically, the kidneys are visualized in their typical retroperitoneal positions, spanning from the T12 to L3 vertebral levels, with the left often slightly higher than the right. The overall shape is bean-like with rounded contours, and uptake is uniformly distributed across the upper, middle, and lower poles, though subtle variations such as slightly more intense uptake in the columns of Bertin or at the poles may occur due to normal renal lobulation. Quantitative assessment reveals balanced differential renal function, with each kidney accounting for 45-55% of total uptake, indicating equivalent contributions to overall renal cortical function. Total renal uptake typically ranges from 40-65% of the injected dose at 2 hours post-administration, reflecting efficient binding to proximal tubular cells in healthy kidneys. Normal variations include minor asymmetries, such as a slight dominance in uptake for one kidney (often the left by 1-2%) in up to 10-15% of cases, potentially influenced by overlying structures like the liver on the right side, though overall symmetry predominates. These findings collectively affirm preserved renal cortical integrity and serve as a baseline for evaluating potential pathology.

Abnormal findings

Abnormal findings on a DMSA scan manifest as deviations from the expected symmetric cortical uptake, revealing underlying renal pathologies through distinct patterns of reduced or absent tracer accumulation. Focal defects appear as wedge-shaped photopenic areas, typically indicating cortical scars or infarcts, which are often located at the poles of the in cases associated with reflux nephropathy. These defects exhibit well-defined margins, parenchymal volume loss, and retraction of the renal contour, distinguishing chronic scarring from acute processes. In acute , multiple small focal defects may be observed, representing areas of with indistinct margins and preserved or slightly increased renal volume, though these can resolve with timely treatment. Global reduction in tracer uptake, affecting an entire kidney, signals severe compromise such as or chronic obstruction, where the affected demonstrates diminished function often below 10% of total renal contribution. This pattern is characterized by overall decreased cortical activity and a smaller size on imaging, potentially bilateral in progressive renal failure. Absent uptake in one kidney is a hallmark of or , where no functional cortical tissue is present, confirming congenital absence or non-viable dysplastic parenchyma. Quantification of these abnormalities enhances diagnostic precision, with regions of interest (ROI) analysis used to calculate differential renal function by comparing uptake between kidneys, ideally within a normal range of 45-55% per side. In cases involving scars, (SPECT) allows for volumetric estimation of defect size, providing a more accurate assessment of parenchymal loss than planar imaging alone. These interpretive patterns often correlate briefly with clinical history, such as , to contextualize the extent of damage.

Advantages and limitations

Clinical benefits

The DMSA scan is the gold standard for identifying parenchymal abnormalities associated with conditions like (VUR) and , with sensitivity reported around 85-90% for cortical scarring in studies compared to pathological findings. This outperforms , which demonstrates sensitivities ranging from 37% to 79% depending on scar severity, with an average around 50% for moderate defects. The superior detection capability allows DMSA to identify small or subtle scars that often misses, enabling earlier intervention to prevent progressive renal damage. Unlike anatomical imaging modalities such as or MRI, which primarily visualize structural changes, the DMSA scan provides essential functional information, including differential renal uptake that quantifies individual contribution to overall function (typically expressed as percentage split). This functional assessment is particularly valuable in pediatric cases, where it guides decisions for congenital anomalies or post-infection without the need for agents or prolonged procedures. In comparison to , DMSA detects smaller scars, with evidence showing DMSA identifying abnormalities in up to 55% of refluxing units versus 38% for . In pediatric populations, DMSA scans are preferred due to their lower , with an effective dose of approximately 1 mSv—substantially less than the 3-10 mSv typical for abdominal scans—while delivering comparable or superior diagnostic yield for scarring. The procedure requires no for most children, as it involves static over 20-30 minutes, facilitating outpatient use and reducing associated costs and logistical burdens compared to sedation-dependent alternatives like dynamic renography. DMSA demonstrates high accuracy in evaluating renal scarring associated with VUR.

Risks and contraindications

The DMSA scan exposes patients to from the technetium-99m-labeled tracer, resulting in a whole-body effective dose of approximately 1 mSv for adults and about 0.9 mSv for children with normal renal function. This radiation level corresponds to a equivalent to 3-6 months of natural exposure, which is lower than that of an abdominal (around 10 mSv). Adverse reactions to the DMSA tracer are uncommon, with manifestations such as urticaria, , pruritus, or reported in rare cases (incidence <1%); these typically resolve without intervention. Injection site complications, including , , or , may occur but are usually mild and self-limiting, managed with local measures like cold compression. The scan is absolutely contraindicated during to avoid fetal , though it may be considered if the clinical benefit clearly outweighs the risk after multidisciplinary consultation. Relative contraindications include acute renal failure, where tracer uptake and imaging accuracy may be compromised, and known to or DMSA components. Risks are mitigated through adherence to the ALARA (as low as reasonably achievable) principle in dosing and imaging protocols, along with patient to facilitate tracer clearance and reduce effective exposure. For breastfeeding individuals, nursing should be paused for approximately 12 hours post-injection, or follow department-specific protocols to minimize infant exposure to the radiotracer. Recent studies (as of 2025) highlight interobserver variability in DMSA interpretation, with disagreements in up to 79% of unusual cases, and emerging non-ionizing alternatives like unenhanced MRI, which show excellent for renal scars, potentially reducing reliance on radiation-based imaging.

Guidelines and standards

Professional recommendations

The (AAP) 2011 clinical practice guideline for the diagnosis and management of initial urinary tract infections (UTIs) in febrile infants and children aged 2 to 24 months does not recommend routine use of dimercaptosuccinic acid (DMSA) scintigraphy following a first febrile UTI, emphasizing instead renal-bladder as the primary imaging modality to identify gross abnormalities. However, DMSA scans are indicated in cases of atypical UTI (e.g., poor response to treatment, septicemia, or non-E. coli organisms), recurrent febrile UTIs, or when reveals abnormalities such as or scarring, particularly in high-risk children under 3 years with risk factors like young age or family history of renal disease. The European Association of Urology (EAU) and European Society for Paediatric Urology (ESPU) guidelines position DMSA scintigraphy as a first-line imaging tool for evaluating renal scarring in children with (VUR), recommending it 4 to 6 months after an acute febrile UTI to assess permanent parenchymal defects, with changes in DMSA uptake correlating to the presence of dilating VUR and risk of breakthrough infections. Similarly, the Society of Nuclear Medicine and Molecular Imaging (SNMMI) and European Association of Nuclear Medicine (EANM) practice guidelines endorse DMSA as the standard for detecting cortical scarring at least 6 months post-UTI in VUR cases, explicitly preferring (SPECT) acquisition over planar imaging for enhanced sensitivity in identifying small defects, particularly in pediatric patients where available. Recent updates to these guidelines from 2020 to 2025, including revisions from EAU/ESPU (2024, with 2025 summary), NICE (2022), and the Indian Society of Pediatric Nephrology (ISPN, 2023), stress a more selective approach to DMSA use in low-risk children to minimize ionizing radiation exposure (approximately 1-2 mSv per scan), prioritizing non-ionizing alternatives like ultrasound or magnetic resonance imaging (MRI) for initial evaluation and reserving DMSA for those with recurrent febrile UTIs, atypical presentations, or confirmed high-grade VUR. The 2024 EAU/ESPU update and 2025 summary maintain recommendations for DMSA in children with recurrent or atypical UTIs to assess renal scarring, performed 4-6 months after the acute infection, with refined risk stratification to further limit unnecessary scans. The UK National Institute for Health and Care Excellence (NICE) guidelines endorse DMSA scintigraphy 4 to 6 months post-infection specifically for children under 16 with recurrent UTIs (defined as two or more upper UTIs or one upper and one or more lower UTIs), and in cases involving grade III or higher VUR to confirm scarring, while advising against acute-phase scans unless clinical suspicion for pyelonephritis persists. These recommendations align with broader radiation safety principles from organizations like the International Commission on Radiological Protection, advocating ALARA (as low as reasonably achievable) exposure in pediatric imaging.

Technical protocols

The EANM and SNMMI joint practice guidelines for renal recommend standardized parameters for planar DMSA imaging to ensure optimal visualization of renal cortical defects. For planar acquisition, a minimum of ,000 counts per view is advised, using a 256 × 256 size and a low-energy high-resolution (LEHR) , with the energy window set at 140 keV ±10% to capture the principal photopeak of 99mTc. These settings apply to posterior and posterior oblique views, acquired 2–6 hours post-injection, promoting consistent image quality across adult and pediatric patients. SPECT acquisition enhances three-dimensional assessment and is recommended, particularly in , with a 360-degree over 120 (3° steps) at 15-20 seconds per using a 128 × 128 . employs ordered subset expectation maximization (OSEM) algorithms with appropriate filters to minimize noise while preserving , typically incorporating 4–8 iterations and 10–16 subsets. Hybrid SPECT/ systems may integrate low-dose for correction, improving quantitative accuracy without significantly increasing . Quality assurance protocols for gamma cameras include daily uniformity checks using a uniform flood source (e.g., 57Co sheet source) to verify integral uniformity within ±3–5% across the field of view, ensuring reliable DMSA image interpretation. Acceptance criteria specify intrinsic better than 8 mm (FWHM) at 140 keV, tested weekly with bar phantoms to confirm system performance prior to clinical use. Pediatric variations adjust for smaller anatomy, such as using pinhole collimators (3–4 mm aperture) in infants for higher , targeting 150,000–300,000 counts per view while maintaining the same energy window and . In all cases, protocols align with standards to minimize dose, such as those from the EANM Dosimetry Committee.

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