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Value of Peptide Receptor Scintigraphy Using ¹²³I-Vasoactive Intestinal Peptide and ¹¹¹In-DTPA-D-Phe1-Octreotide in 194 Carcinoid Patients: Vienna University Experience, 1993 to 1998

From the Departments of Internal Medicine I, Nuclear Medicine, Internal Medicine III, Internal Medicine IV, Surgery, and Radiology, University of Vienna, and Research Center Seibersdorf, Vienna, Austria.

Address reprint requests to Irene Virgolini, MD, Department of Nuclear Medicine, University of Vienna, Waehringer Guertel 18-20, A-1090 Vienna, Austria; email irene.virgolini{at}akh-wien.ac.at

	ABSTRACT

TOP ABSTRACT INTRODUCTION PATIENTS AND METHODS RESULTS DISCUSSION REFERENCES

 
PURPOSE: To report our experience with both ¹²³I-vasoactive intestinal peptide (VIP) and ¹¹¹In-DTPA-D-Phe¹-octreotide for imaging to identify primary and metastatic tumor sites in carcinoid patients.

PATIENTS AND METHODS: One hundred ninety-four patients with a verified or clinically suspected diagnosis of a carcinoid tumor were injected with ¹¹¹In-DTPA-D-Phe¹-OCT for imaging purposes, while 133 patients underwent scanning with both ¹²³I-VIP and ¹¹¹In-DTPA-D-Phe¹-OCT in random order. Imaging results were compared with computed tomography scans, results of conventional ultrasound, endosonography, and endoscopy, and results of surgical exploration in case of inconclusive conventional imaging.

RESULTS: Primary or recurrent carcinoid tumors could be visualized with ¹¹¹In-DTPA-D-Phe¹-OCT in 95 (91%) of 104 patients; metastatic sites were identified in 110 (95%) of 116 patients. In 11 (51%) of 21 patients with suggestive symptoms but without identified lesions by conventional imaging, focal tracer uptake located the carcinoid tumor. In addition, metastatic disease was demonstrated in three patients after resection. In a direct comparison in the 133 patients who underwent both imaging modalities, ¹¹¹In-DTPA-D-Phe¹-OCT was found to be superior to ¹²³I-VIP, with 35 (93%) of 38 versus 32 (82%) of 38 scans being positive in primary or recurrent tumors, 58 (90%) of 65 versus 53 (82%) of 65 being positive in patients with metastatic sites, and seven (44%) of 16 versus four (25%) of 16 being positive in patients with symptoms but otherwise negative work-ups. Overall, additional lesions not seen on conventional imaging were imaged in 43 (41%) of 158 versus 25 (25%) of 103 scans with ¹¹¹In-DTPA-D-Phe¹-OCT and ¹²³I-VIP, respectively.

CONCLUSION: Both peptide tracers have a high sensitivity for localizing tumor sites in patients with ascertained or suspected carcinoid tumors, with ¹¹¹In-DTPA-D-Phe¹-OCT scintigraphy being more sensitive than ¹²³I-VIP receptor scanning. Both, however, had a higher diagnostic yield than conventional imaging, as verified by surgical intervention or long-term follow-up. The combination of both peptide receptor scans does not seem to further enhance diagnostic information.

	INTRODUCTION

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NEUROENDOCRINE TUMORS are rare disease entities, often presenting as bizarre diagnostic puzzles.¹ The fact that such malignancies arise from hormonally active cells explains the wide variety of symptoms encountered in patients with neuroendocrine cancers of various origin. The different manifestations are related to the release of hormones or other biologically active substances produced in excessive amounts by the tumor, including insulin, gastrin, vasoactive intestinal peptide (VIP), glucagon, and serotonin.^2-4 Such cancers constitute a group of relatively slow-growing malignancies, which are sometimes diagnosed only after years of symptoms. This is due to the fact that the amount of hormones secreted does not necessarily correlate with tumor size, whereas small cancers tend to escape clinical detection by means of conventional radiologic imaging.^5-7 Thus, the initiation of successful therapy or symptomatic palliation is often delayed in such patients.

Carcinoid tumors constitute the group with the highest incidence among all cases of neuroendocrine malignancies, predominantly arising in the gastrointestinal (GI) tract but also in various other anatomic sites.⁸ According to epidemiologic data, carcinoids of the GI tract occur at a rate of 1.5 cases per 100,000 people per year.⁹ As has been stated, the onset of symptoms related to excessive serotonin production, summarized under the term carcinoid syndrome, may precede the correct diagnosis and localization of the tumor by years. While long-term symptomatic control of tumor-related symptoms can be achieved in some patients by noninvasive means, the treatment of choice, at least in localized disease, remains surgical resection because it is the only measure to offer potential cure. On the other hand, the removal of the primary cancer in the absence of symptoms such as bowel obstruction does not significantly alter the prognosis in patients with disseminated disease.

In vitro data have demonstrated a high amount of receptors for various hormones and peptides on malignant cells of neuroendocrine origin, including carcinoid tumors.¹⁰ Among the latter, binding sites for members of the somatostatin (SST) family (SST receptors/1 through 5) are frequently found, and their expression has led to therapeutic and diagnostic attempts to specifically target these receptors. According to findings in patients with tumors arising from endocrine-active cells,^11-14 the use of radiolabeled octreotide (OCT) for imaging purposes has been incorporated into the clinical work-up of patients suspected of having neuroendocrine tumors.

VIP is a peptide consisting of 28 amino acids displaying a broad range of biologic activities.¹⁵ Apart from its vasodilatory properties, it has been implicated in the promotion of growth and proliferation of normal as well as malignant tissues.^16,17 These effects are also mediated via cell-surface receptors (VIPR). Large numbers of VIPR are expressed on a variety of tumors, including adenocarcinomas,¹⁸ breast cancer tumors,¹⁹ and endocrine tumors.^20,21 In addition, our own data suggest a significant cross-competition between SST and VIP on the cellular level,²⁰ which might be the result of binding to SSTR3.²² Based on these findings, a peptide receptor scan using radioiodinated VIP as a tumor-seeking agent has been developed and successfully applied at the University of Vienna in patients with various types of cancer.^21,23-27

In this article, we report our experience with both ¹¹¹In-DTPA-D-Phe¹-OCT and ¹²³I-VIP in 194 consecutive patients with histologically verified or clinically suspected carcinoid tumors admitted to our institution between January 1993 and December 1998.

	PATIENTS AND METHODS

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Patients
A total of 194 patients with a median age of 63 years (range, 43 to 79 years) with verified carcinoid tumors or clinically suspected malignancy were admitted to our institution between 1993 and 1998 (Table 1). In 158 patients, a histologic diagnosis had been established before application of radiotracers, while 21 patients were believed to have a carcinoid tumor on the basis of symptoms (diarrhea alone in 13 patients, diarrhea accompanied by flushing in five patients, and flushing alone in three patients), an elevated level of urinary 5-hydroxyindoleacetic acid (5-HIAA), and no lesions indicating the site of malignancy on conventional computed tomography (CT) scans or different staging methods, including sonography, endoscopy, and endosonography. In addition, 15 patients were admitted to our institution after resection of a carcinoid tumor that was found during appendectomy or rectoscopy; they were thought to be free of tumor at the time of imaging. In total, 42 patients had primary tumors alone, whereas 62 had metastases along with their primary tumor. Histologic verification of at least one of these lesions was performed before surgery, and additional biopsies were attempted only in cases of lesions with uncharacteristic radiologic features or the absence of clear progression on consecutive CT scans performed at an interval of at least 3 months. In 54 cases, metastases were diagnosed after resection of the primary tumor, and histologic verification of biopsy specimens was performed in 26 patients, whereas in 15 patients, the appearance of new lesions on CT scans along with the development of clinical symptoms (accompanied by a rise in 5-HIAA in 11 cases) was rated diagnostic for relapse. In the additional 13 cases, only the appearance of new lesions progressing on a second CT investigation performed between 3 to 6 months later was present, and five of these patients also had elevated 5-HIAA levels without symptoms.

When results of scintigraphic imaging corresponded with those of conventional imaging or surgery, or when a corresponding lesion appeared on conventional imaging during the follow-up period, lesions were rated as true-positive. Lesions not detected on scintigraphy but seen on conventional imaging (and showing progression during the follow-up period) and surgically detected tumors verified by histologic examination without a corresponding "hot spot" were rated as false-negative. False-positive results were defined as hot spots on gamma-camera imaging rated suggestive for a malignant process without a corresponding result on conventional imaging within the follow-up period or on surgical exploration.

Preparation of Radioiodinated VIP
The preparation of ¹²³I-VIP has been described earlier.^13,14 In brief, VIP was generated by a peptide-synthesizing machine and labeled with ¹²³I using a modified iodogen method. ¹²³I-VIP was purified by preparative high-pressure liquid chromatography (column: RP C18, 5 µm, 4 x 250 mm; eluent: 74% [vol/vol] aqueous 0.25 mol/L triethylammoniumformiate, pH 3, 26% [vol/vol] acetonitrile at 1 mL/min) to obtain a high specific activity. The column eluent passed through a scintillation radioactivity detector and ultraviolet (280-nm) detector in a series. The system was calibrated with unlabeled VIP and enabled collection of pure radioiodinated VIP, separated from unlabeled VIP, reagents, and inorganic iodine species. The eluent was evaporated at reduced pressure. The product was dissolved in phosphate-buffered saline containing 0.1% (wt/vol) Tween 80 (Koch-Light Lab Ltd, Colnbroke, United Kingdom). The labeled product was analyzed by analytical high-pressure liquid chromatography (corresponding to the preparative system, however, using a dedicated analytical column) and zone electrophoresis (Whatman 3 MM paper [Whatman, Maidstone, United Kingdom], 0.1 barbital buffer, pH 8.6, using a field of 300 V for 10 minutes). The percentage of unbound iodine (< 3% in all preparations) remained stable for at least 24 hours. Before injection, ¹²³I-VIP was filtered through sterile Millex GV 0.2-µm membranes (Millipore, Milford, MA). As has previously been published,^21,22 radioiodination does not affect binding of ¹²³I-VIP to respective binding sites, as routinely assessed by in vitro binding studies for quality control before application of the tracer. ¹²³I-VIP was administered as a single intravenous bolus injection in 3 mL of 0.9% sodium chloride solution (150 to 200 MBq; ~ 1 µg) of VIP) after thyroid gland blockade with potassium iodide and perchlorate in all patients.

Preparation of Radiolabeled OCT
For imaging purposes, the commercially available ¹¹¹In-DTPA-D-Phe¹-OCT (OctreoScan; Mallinckrodt Medical, Northhampton, United Kingdom) was used. DTPA-D-Phe¹-OCT 10 µg was labeled with 120 to 150 MBq ¹¹¹InCl₃, according to the manufacturer’s instructions.

Gamma-Camera Imaging and Analysis
¹²³I-VIPR scintigraphy. Planar and single photon emission tomography (SPET) acquisitions were performed with a large field-of-view gamma-camera equipped with a low-energy parallel-hole collimator. In most patients, sequential abdominal images were recorded every minute for 30 minutes (matrix, 128 x 128 pixels). Thereafter, planar images in anterior, posterior, and lateral views of three regions covering the brain and neck, thorax, and abdomen were acquired at 30 minutes and 2 to 4 hours (and in initial studies at 18 to 24 hours) after injection (matrix, 256 x 256 pixels; 300 to 800 kcounts were acquired). For recording and visualization, standard techniques were used. A three-headed (Picker Prism 3000; Picker Medical Imaging, Cleveland, OH) or one-headed gamma-camera (Picker Prism 1000) was used for SPET imaging at 2 to 4 hours. Scanning was performed in a 360° circle in 6° steps, 30 seconds per step. After being processed by a dedicated computer (backprojection with a ramp filter, postfiltering with a low-pass filter), the data were reconstructed in three planes (coronal, sagittal, and transaxial reconstruction).

¹¹¹In-DTPA-D-Phe¹-OCT scintigraphy. For planar and SPET studies, a large field-of-view gamma-camera (Toshiba America Medical Systems, Inc, Tustin, CA) equipped with a medium-energy general-purpose collimator was used. At the time of injection, the field of view covered the abdomen and some of the thorax. For recording and visualization, standard techniques were used. Sequential images were recorded every minute, starting immediately after the injection for 30 minutes (matrix, 128 x 128 pixels). Planar images in anterior, posterior, and lateral views were acquired at 30 minutes, between 3 and 6 hours, between 18 and 24 hours, and at approximately 72 hours after intravenous injection covering the brain and neck, thorax, and abdomen (matrix, 128 x 128 pixels; 150 to 300 kcounts; scanning time, 10 to 20 minutes). SPET acquisition was performed in all patients between 18 and 24 hours and at 48 hours after injection. Both energy peaks were used for scanning (set at 173 keV and 247 keV) with a 20% window. SPET imaging was done in a 360° circle, using 6° steps, 30 seconds per step. After being processed by a dedicated computer (prefiltering with a Wiener filter, postfiltering with a ramp filter), the data were reconstructed in three planes (slice thickness of 7 mm). All scans were viewed by at least two nuclear medicine physicians with no knowledge of the extent of tumor spread. A yes-or-no system was used to evaluate the presence of primary tumors and metastases as judged both by planar and SPET reconstructions.

	RESULTS

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¹¹¹In-DTPA-D-Phe¹-OCT Scintigraphy
Overall, a high sensitivity for both primary and metastatic tumors was obtained in our series with application of ¹¹¹In-DTPA-D-Phe¹-OCT, irrespective of organ site and lesion size. In total, primary or recurrent carcinoid tumors could be visualized by means of ¹¹¹In-DTPA-D-Phe¹-OCT in 95 (91%) of 104 patients. Metastatic sites were identified in 110 (95%) of 116 patients, corresponding to 325 (88%) of 374 lesions. Overall, lesions not seen on initial conventional staging were encountered in 79 (41%) of 194 patients. In 11 (51%) of 21 patients with suggestive symptoms and elevated 5-HIAA levels exceeding 20 mg/mL but without identified lesions by conventional imaging, focal tracer uptake identified the location of the carcinoid tumor. This was confirmed in all cases by histologic evaluation after surgery. However, of the 10 remaining patients scheduled for a repeat imaging, six were lost to follow-up and four patients did not return for another ¹¹¹In-DTPA-D-Phe¹-OCT scan but underwent surgery for increasing symptoms of bowel obstruction. In all four patients, a carcinoid tumor could be pathologically demonstrated after surgery. In addition, the presence of metastatic disease was demonstrated in three patients thought to be free of tumor after resection, which was also confirmed during second-look surgical intervention.

Concerning the time of imaging, the highest diagnostic accuracy was observed with SPET reconstructions performed 24 hours after injection of the tracer. SPET studies performed 48 hours after injection did not result in a higher diagnostic yield (Fig 1).

View larger version (117K): [in this window] [in a new window]   Fig 1. SPET reconstruction (transversal slices; slice thickness, 7 mm) shows corresponding images of 111In-DTPA-D-Phe1-OCT scintigraphy (A) and 123I-VIPR scanning (B). SPET studies were performed 6 hours after injection (A) and 4 hours (B) after injection of the respective tracer, depicting focal tracer accumulation in two neighboring sites (arrow) corresponding to surgically verified liver metastases in a 56-year-old male patient.

Direct comparison showed superior results with ¹¹¹In-DTPA-D-Phe¹-OCT: 42 (93%) of 45 v 38 (84%) of 45 scans were positive for primary or recurrent tumors, 83 (90%) of 92 v 76 (82%) of 92 scans were positive in patients with metastatic sites, and seven (43%) of 16 v four (25%) of 16 scans were positive in patients with symptoms and elevated 5-HIAA levels but otherwise negative work-ups. Identification of additional and as yet unknown lesions was possible in 38 (37%) of 104 patients. On a per-lesion basis, ¹¹¹In-DTPA-D-Phe¹-OCT visualized 134 (92%) of 146 known liver metastases, 37 (89%) of 42 lymph node lesions, 19 (100%) of 19 lung lesions, and 23 (88%) of 26 bone lesions.

	DISCUSSION

TOP ABSTRACT INTRODUCTION PATIENTS AND METHODS RESULTS DISCUSSION REFERENCES

 
The finding that neuroendocrine tumors express high amounts of SSTR had led to the development of radiolabeled OCT, which has demonstrated its ability to localize such tumors in large cohorts of patients.^11-14 As has been published, this agent interacts preferentially with SSTR subtypes 2 and 5, which are expressed in relatively high amounts in most neuroendocrine tumors. In addition, a high density of binding sites for VIP could be found in vitro in cell lines and human tumor samples, and our first in vivo series have underscored the potential of ¹²³I-VIP for visualizing neuroendocrine tumors and metastases.^21,23-27 On the basis of these initial data, we performed a study to compare directly the diagnostic capability of both labeled peptides.

Our data confirm that peptide receptor scintigraphy plays an important role in the detection and staging of carcinoid tumors. Both tracers applied in our study displayed the potential to localize primary as well as metastatic lesions, even in cases with no evidence of disease on conventional work-up. As could be expected from our initial series,^18,19 VIPR scintigraphy had a high sensitivity for primary tumors (84%) and metastases (82%). In addition, four of 16 patients with symptomatic disease but otherwise negative conventional work-ups had their tumors located by the novel peptide tracer.

However, superior diagnostic results were obtained with the application of ¹¹¹In-DTPA-D-Phe¹-OCT. A more than 90% sensitivity both for primary and metastatic lesions was found in our patients, and six of 21 patients without lesions documented with conventional staging methods had positive scans in the presence of symptoms and elevated 5-HIAA levels.

A direct comparison of both tracers in 133 patients showed a sensitivity of 93% versus 83% in patients with primary and recurrent lesions, respectively, while metastases could be imaged in 90% of patients as compared with 82% with VIP.

As could be expected from pharmacokinetic data,^18,19 one of the major shortcomings of ¹²³I-VIP is its inability to visualize small pulmonary lesions. In fact, about 40% of the tracer is trapped in the lung a few minutes after application,¹⁹ providing a high rate of physiologic background. Thus, small tumors or lesions with a low receptor density cannot be distinguished from normal lung uptake. In fact, ¹¹¹In-DTPA-D-Phe¹-OCT, which is not trapped in the lungs, demonstrated a striking superiority for imaging of lung lesions, whereas less than 50% of pulmonary deposits could be seen on VIPR scintigraphy. Both imaging methods, however, showed comparable performance for target lesions located in the liver, irrespective of lesion size.

Given the overall results, ¹¹¹In-DTPA-D-Phe¹-OCT is the tracer of choice to date for diagnosis in patients with suspected carcinoids or for staging in patients with verified carcinoid tumors. Our data are also in line with the findings published by Krenning et al,^28,29 who found a high sensitivity for various types of neuroendocrine tumors, including carcinoids. These findings as well as our results nevertheless seem to be superior to other series published in the literature.^30,31 As has already been pointed out,^28,29 this might be related to differences in scanning procedures as well as to the routine performance of SPET studies of both the thorax and abdomen in all patients, as performed by Krenning et al as well as in this study. Nevertheless, evaluation of new compounds to further improve diagnostic accuracy is still warranted, since 10% to 15% of lesions are apparently missed with the application of radiolabeled OCT, even with state-of-the-art SPET studies as routinely performed in our series in all patients.

We conclude that both tracers are able to visualize carcinoid tumors with a higher sensitivity compared with conventional imaging. However, our results indicate that ¹¹¹In-DTPA-D-Phe¹-OCT is superior to ¹²³I-VIPR scintigraphy for imaging of carcinoid tumors.

	REFERENCES

TOP ABSTRACT INTRODUCTION PATIENTS AND METHODS RESULTS DISCUSSION REFERENCES

 
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Submitted April 23, 1999; accepted November 16, 1999.

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