Comparison of Ga-68-Labeled Fusarinine C-Based Multivalent RGD Conjugates and [(68)Ga]NODAGA-RGD-In Vivo Imaging Studies in Human Xenograft Tumors.

PURPOSE: Multimeric arginine-glycine-aspartic acid (RGD) peptides have advantages for imaging integrin αvβ3 expression. Here, we compared the in vitro and in vivo behavior of three different Ga-68-labeled multimeric Fusarinine C-RGD (FSC-RGD) conjugates, whereby RGD was coupled directly, via a succinic acid or PEG linker (FSC(RGDfE)3, FSC(succ-RGD)3, FSC(Mal-RGD)3). The positron emission tomography/X-ray computed tomography (PET/CT) imaging properties were further compared using [(68)Ga]FSC(succ-RGD)3 with the monomeric [(68)Ga]NODAGA-RGD in a murine tumor model. PROCEDURE: FSC-RGD conjugates were labeled with Ga-68, and stability properties were studied. For in vitro characterization, the partition coefficient, integrin αvβ3 binding affinity, and cell uptake were determined. To characterize the in vivo properties, biodistribution studies and microPET/CT were carried out using mice bearing either human M21/M21-L melanoma or human U87MG glioblastoma tumor xenografts.
RESULTS: All FSC-RGD conjugates were quantitatively labeled with Ga-68 within 10 min at RT. The [(68)Ga]FSC-RGD conjugates exhibited high stability and hydrophilic character, with only minor differences between the different conjugates. In vitro and in vivo studies showed enhanced integrin αvβ3 binding affinity, receptor-selective tumor uptake, and rapid renal excretion resulting in good imaging properties.
CONCLUSIONS: The type of linker between FSC and RGD had no pronounced effect on targeting properties of [(68)Ga]FSC-RGD trimers. In particular, [(68)Ga]FSC(succ-RGD)3 exhibited improved properties compared to [(68)Ga]NODAGA-RGD, making it an alternative for imaging integrin αvβ3 expression.

Introduction

Integrins are a family of cation-dependent heterodimeric transmembrane adhesion receptors which are involved in cell-cell, cell-extracellular matrix, and cell-pathogen interactions. They are expressed on a variety of cell types and play an important role in many aspects of tumor development such as tumor-induced angiogenesis, tumor proliferation, and tumor cell migration [1]. Optimized cyclic pentapeptides containing the arginine-glycine-aspartic acid (RGD) motif show high affinity for the integrin αvβ3 as well as remarkable metabolic stability [2, 3]. Versatile RGD-based sequences, acyclic or cyclic, have been labeled with halogens as well as with various radiometals to noninvasively determine the integrin αvβ3 expression [4, 5]. Further studies have demonstrated that multimerization of the RGD motif, i.e., combination of several RGD sequences in one single molecule, can increase binding affinity leading to enhanced target uptake and slower clearance from the targeted tumor [6]. The first successful example allowing noninvasive imaging of integrin αvβ3 expression is [18F]Galacto-RGD, which has been tested in preclinical studies and clinical trials with good pharmacokinetics and receptor-specific uptake [7-10]. However, the common problem encountered for F-18 labeling is the complex and time-consuming synthesis of these tracers with moderate yield limiting routine use in the clinical setting.

To achieve an easier and more rapid radiosynthesis, with high specific activity and high yield of the desired radiotracer, an alternative approach is direct labeling with radiometals. Therefore, the RGD peptides were modified with corresponding chelator systems and radiolabeled with appropriate radiometals such as Ga-68, Cu-64, Y-86, and Zr-89 for positron emission tomography (PET) imaging or Tc-99m and In-111 for single-photon emission computed tomography (SPECT) imaging. Of the nuclides mentioned above, Ga-68 has received tremendous attraction as a PET radionuclide due to the ready availability from 68Ge/68Ga generator systems and its physical characteristics with a half-life of 68 min and a high positron yield of 89 %. This half-life is compatible with the pharmacokinetics of many peptides including RGD peptides. As a result of its significance for PET imaging, several bifunctional chelators have been employed for Ga-68 labeling of biomolecules including the most widely used cyclic 1,4,7,10-tetraazacyclododecane-1,4,7,10-tetraacetic acid (DOTA) derivatives as well as 1,4,7-triaazacyclononane-1,4,7-triacetic acid (NOTA) derivatives (e.g., NODAGA, 1,4,7-triazacyclononane-1,4-bis(acetic acid)-7-(2-glutaric acid)), of which the later are better suited for the small Ga3+ ion due to their smaller cavity size. The higher complex stability constant of the NOTA system allows radiolabeling even at room temperature (RT) within minutes. [68Ga]NODAGA-RGD is one promising monomeric compound showing excellent in vitro and in vivo properties [11, 12]. Recently, a multivalent bifuncational chelator named 1,4,7-triazacyclononane-1,4,7-tris[(2-carboxyethyl)methylenephosphinic acid] (TRAP) was developed and Ga-68-labeled TRAP(RGD)3 was reported to further improve integrin αvβ3 targeting as compared to [68Ga]NODAGA-RGD [13]. Recently, we reported that fusarinine C (FSC), a cyclic hydroxamate siderophore, is a promising Ga-68 and Zr-89 binding bifunctional chelator [14-17]. FSC possesses three primary amine functions allowing conjugation of up to three targeting vectors, thereby facilitating the application of the multimerization approach. FSC-based multimeric RGD conjugates (FSC(succ-RGD)3, FSC(RGDfE)3, and FSC(Mal-RGD)3) were previously synthesized via different conjugation strategies [14, 16]. In vitro and in vivo evaluation of Zr-89-labeled FSC-RGD conjugates demonstrated the superiority of FSC as a bifunctional chelator for Zr-89 as well as the receptor specificity of [89Zr]FSC-RGD conjugates [16]. However, the long physical half-life of Zr-89 (78.4 h) may be considered nonideal for the biological half-lives of small RGD peptides which range from several minutes to hours. By contrast, the 68-min half-life of Ga-68 matches well with the biological half-lives of the cyclic RGD peptides. As an excellent Ga-68 chelator, FSC complexation of Ga-68 occurs at RT resulting in high RCP and specific activity within minutes [15].

In this study, FSC(succ-RGD)3, FSC(RGDfE)3, and FSC(Mal-RGD)3 were labeled with Ga-68 and the comparison of in vitro and in vivo properties including PET/CT imaging of these compounds in a human melanoma tumor model is reported for the first time. PET/CT imaging properties of [68Ga]FSC(succ-RGD)3 were further compared with the monomeric [68Ga]NODAGA-RGD in an alternative human glioblastoma tumor model.

Materials and Methods

General

All described substances and solvents were of reagent grade and were used without further purification. FSC(succ-RGD)3, FSC(RGDfE)3, and FSC(Mal-RGD)3 were synthesized as described earlier [16]. Milli-Q water was used for preparing all reagent solutions. Human melanoma M21 and M21-L cells were a kind gift from D. A. Cheresh (Department of Pathology and the Moores Cancer Center, University of California San Diego, La Jolla, CA, USA), and human glioblastoma U87MG cells were obtained from American Type Culture Collection (ATCC, Manassas, VA, USA). Elution of the Ga-68 generator (IGG100, Eckert & Ziegler Strahlen- und Medizintechnik AG, Berlin, Germany, nominal activity 1850 MBq) was performed with 0.1-M HCl solution (Rotem Industries Ltd., Beer-Sheva, Israel).

High-Performance Liquid Chromatography

An UltiMate 3000 (Thermo Fisher Scientific, Vienna, Austria) high-performance liquid chromatography (HPLC) system consisting of an UltiMate 3000 RS pump, a column oven (temperature setting 25 °C) UV-vis variable wavelength detector (220 nm), and a radioactivity detector (Raytest GABI, Raytest, Straubenhardt, Germany) was used; gradient: acetonitrile (CH3CN)/H2O/0.1 % trifluoroacetic acid (TFA) gradient: 0–0.5 min 0 % CH3CN, 0.5–7.0 min 0–55 % CH3CN

Ga-68 Radiolabeling

The fraction containing the highest Ga-68 activity (approximately 400–500 MBq in 0.1 M HCl) was collected, and 110 μl 1.9-M NaOAc solution was added to adjust pH to 4.5. After briefly shaking, 100 μl of the corresponding solution was mixed with 30 μl of the FSC-RGD conjugates (1 μg/μl in water; FSC(succ-RGD)3, 10.8 nmol; FSC(RGDfE)3, 12.0 nmol; or FSC(Mal-RGD)3, 7.9 nmol) and incubated at RT for 10 min. Analytical HPLC was used to confirm quantitative labeling. Subsequently, the labeling solution was diluted with phosphate‐buffered saline (PBS) and used for in vitro and in vivo studies without further purification.

The labeling of NODAGA-RGD with Ga-68 was carried out as described previously [11]. Briefly, to 100 μl of Ga-68 eluate (approximately 40–50 MBq in 0.1 M HCl), 10 μl of NODAGA-RGD (1 μg/μl in water, 10.4 nmol) was added and the pH of the reaction solution was adjusted to 5 using 1.9-M NaOAc solution. The solution was allowed to react for 15 min at RT. Subsequently, the labeling solution with a radiochemical yield (RCY) higher than 96 % was diluted with PBS and used without further purification.

Stability Studies

The stability of [68Ga]FSC(succ-RGD)3, [68Ga]FSC(RGDfE)3, and [68Ga]FSC(Mal-RGD)3 was evaluated by incubating the radiotracers in PBS, EDTA solution (pH 7; >1000-fold molar excess of EDTA), and fresh human serum for up to 120 min, respectively. At selected time points, aliquots of PBS or EDTA solution were analyzed directly via RP-HPLC, while serum aliquots were mixed with equal volumes of CH3CN, vortexed, and centrifuged at 20,000 relative centrifugal force (rcf) for 2 min. Before analysis, the precipitate was washed three times using CH3CN.

Distribution Coefficient (logD)

A volume of 500 μl PBS including 0.5 MBq radioligand (approximately 0.5 μg peptide) was combined with 500 μl octanol; the mixture was vortexed for 15 min and centrifuged for 2 min at 2000 rcf. From each phase, an aliquot (50 μl) was pipetted out and measured in a 2480 Wizard2 Automatic Gamma Counter (PerkinElmer, Vienna, Austria). Each measurement was repeated five times. LogD value was calculated as the average log ratio of the radioactivity in the organic fraction and the PBS fraction.

Binding Affinity for Immobilized Integrin αvβ3 (Half Maximal Inhibitory Concentration Value)

In vitro binding affinities of cyclo(-Arg-Gly-Asp-DTyr-Val-) (c(RGDyV)) and the three FSC-RGD conjugates were determined by using isolated integrin αvβ3 (Millipore-Chemicon, Temecula, CA, USA) and I-125-labeled c(RGDyV) as radioligand. ([125I]c(RGDyV) was produced as described in [18]). To integrin αvβ3, coated overnight at 4 °C onto 96-well plates (Nunc, Thermo Fisher Scientific, Vienna, Austria), [125I]c(RGDyV) and the corresponding peptides in increasing concentrations from 0.001 to 100 nM were added. Plates were washed, and integrin bound activity was recovered with 2-M NaOH solution and counted in a gamma counter. OriginPro 8.5 software (Northampton, MA, USA) was used to calculate half maximal inhibitory concentration (IC50) values in three independent measurements.

Cell Culture

All cell lines were grown to confluence at 37 °C in a humidified atmosphere of 95 % air/5 % carbon dioxide and split approximately every 48 h. U-87 MG cells were cultured in tissue culture flasks (Cellstar®; Greiner Bio-One, Kremsmuenster, Austria) using EMEM supplemented with 10 % volume/volume (v/v) heat-inactivated fetal bovine serum (FBS), 1 % v/v penicillin/streptomycin/glutamine solution (PSG), 1 % v/v sodium pyruvate solution, and 1 % v/v nonessential amino acid solution. M21 cells were grown using DMEM supplemented with 10 % v/v FBS and 1 % v/v PSG solution. M21-L cells were maintained in germ count dishes (Greiner Bio-One) in RPMI 1640 cell culture medium containing 10 % FBS and 1 % PSG.

Internalization Assay

M21 cells (integrin αvβ3 positive) were diluted with RPMI 1640 (Gibco, Invitrogen Corporation, Paisley, UK) containing 1 % glutamine (m/v), 1 % bovine serum albumin (BSA) (m/v), CaCl2 (1 mM), MgCl2 (1 mM), and MnCl2 (10 mM) to a concentration of 2.0 × 106 cells/ml. One-milliliter aliquots in Eppendorf tubes were incubated at 37 °C for 1 h in triplicates, and [68Ga]FSC(succ-RGD)3, [68Ga]FSC(RGDfE)3, or [68Ga]FSC(Mal-RGD)3 (approximately 1.5 × 106 cpm, 1.2 μg peptides) in PBS with 0.5 % BSA (150 μl, total series) or with 10 μM c(RGDyV) in PBS/0.5 % BSA (150 μl, nonspecific series) at 37 °C was added. After 90-min incubation was stopped by centrifugation, the medium was removed followed by washing (twice) with ice-cold Tris-buffered saline. After incubation in acid wash buffer (20 mM acetate buffer, pH 4.5) at 37 °C for 5 min (two times) and centrifugation, membrane bound activity was collected in plastic vials. Internalized radioligand fraction was collected after lysing cells by addition of 2 M NaOH. The internalized activity was expressed as percentage of total activity per milligram protein after spectrophotometric determination of protein (Bradford assay) in the NaOH fraction.

Ex Vivo Biodistribution Studies

All animal experiments were approved by the Austrian Ministry of Science (BMWF-66.011/000604-II/3b/2012 and BMWFW-66.011/0049-WF/II/3b/2014) and the Czech Ministry of Education Youth and Sports (MSMT-22421/2013-12) as well as by the institutional Animal Welfare Committee of the Faculty of Medicine and Dentistry of Palacky University in Olomouc and conducted in compliance with the Austrian and Czech animal protection laws.

For the induction of tumor xenografts, female, athymic BALB/c nude mice (Charles River Laboratories) were injected subcutaneously with either 5 × 106 integrin αvβ3-positive M21 cells into the right hind limb and with 5 × 106 integrin αvβ3-negative M21-L cells (negative control) into the left hind limb of the same mouse. Approximately 3 weeks after inoculation, the tumors had reached a volume of 0.3–0.6 cm3. On the day of the experiment, [68Ga]FSC(succ-RGD)3, [68Ga]FSC(RGDfE)3, or [68Ga]FSC(Mal-RGD)3 (∼0.5 MBq/mouse, ∼0.5 μg peptide, respectively) was intravenously injected in the lateral tail vein. Mice were euthanized by cervical dislocation at 1 and 2 h (only for [68Ga]FSC(succ-RGD)3) after injection. Organs (spleen, pancreas, stomach, intestine, kidney, liver, heart, and lung), blood, muscle tissue, and tumors were dissected and weighed. Activity of the different samples was measured in the gamma counter. Results were expressed as percentage of injected dose per gram tissue (% ID/g).

MicroPET/CT Imaging

To compare the imaging properties of [68Ga]FSC(succ-RGD)3, [68Ga]FSC(RGDfE)3, and [68Ga]FSC(Mal-RGD)3, microPET/CT imaging experiments were conducted on an Inveon microPET/CT scanner (Siemens Preclinical Solutions, Knoxville, USA). BALB/c nude mice bearing M21-positive tumor xenografts were administered with [68Ga]FSC(succ-RGD)3 (or [68Ga]FSC(RGDfE)3, [68Ga]FSC(Mal-RGD)3, ∼5 MBq/mouse, ∼5 μg peptide) via intravenous (i.v.) injection. The body temperature of mice was maintained at 37 °C on the scanner bed and in the incubation chambers using heating pads. Dynamic 10-min duration PET scans were performed for 50 min while static PET scans (10 min) were performed at 1-h post-injection (p.i.), followed by a 25-min CT scan (spatial resolution, 113 μm; 80 kV, 500 mA). The mice remained under general anesthesia (isoflurane/O2) during the time between injection and imaging. The microPET/CT scans were reconstructed with Inveon Acquisition Workplace software (version 1.5; Siemens Preclinical Solutions), using a three-dimensional fast maximum a posteriori algorithm with the following parameters: matrix 256 × 256 × 161; pixel size 0.4 × 0.4 × 0.8 mm, and β-value of 1.5-mm resolution with uniform variance. Spherical isocontours were set at 50 % of the maximal pixel value to measure uptake values (Bq/ml) in kidneys, heart, and tumor.

To investigate the capabilities of binding to the integrin αvβ3 receptors in the different tumor xenograft models and, at the same time, compare the imaging properties of [68Ga]FSC(succ-RGD)3 and [68Ga]NODAGA-RGD, two U87MG tumor-bearing mice were administered retro-orbitally (r.o.) [19] under general anesthesia with [68Ga]FSC(succ-RGD)3 and [68Ga]NODAGA-RGD each other (∼6 MBq/mouse, ∼5 μg peptide) at continued days. For the induction of tumor xenografts, female, athymic BALB/c nude mice (AnLab, Prague, Czech Republic) were injected subcutaneously with 5 × 106 U87MG cells into the right flank. The tumors were allowed to grow until they had reached a volume of 0.5 to 0.8 cm3. Imaging experiments were conducted on an Albira microPET/SPECT/CT imaging system (Bruker Biospin Corporation, Woodbridge, CT, USA). MicroPET/CT images were acquired under general anesthesia (isoflurane/O2) and heating at 37 °C. PET data for each mouse was recorded via either dynamic imaging for 90 min (5-min PET scan per frame) or static scans (a 5-min PET scan (axial FOV 148 mm) was performed, followed by a 25-min CT scan (axial FOV 65 mm, 45 kVp, 400 μA, at 600 projections)) at 90 min p.i. The microPET/CT scans were reconstructed with Albira software (Bruker Biospin Corporation, Woodbridge, CT, USA) using maximum likelihood expectation maximization (MLEM) and filtered backprojection (FBP) algorithms. Dead time, decay correction, attenuation correction, and normalization were applied to all PET data. The uptake values (%ID/g) in kidneys, heart, and tumor were analyzed by drawing standardized volumes of interest.

Statistical Analysis

Statistical analysis was performed using SPSS 17.0 software. The biodistribution data was analyzed using Student’s t test. The level of significance was set at P < 0.05.

Results

Radiolabeling and Stability Studies

All FSC-RGD conjugates were labeled with Ga-68 using NaOAc buffer at pH 4.5 at RT within 10 min resulting in almost quantitative labeling efficiency (>98 %) and specific activities ranging from 2.5 to 4 GBq/μmol. For all experiments, the labeling solution was used without further purification. Stability studies revealed high stability for all three compounds in all examined media for up to 2 h, indicating that the different conjugation strategies had no detectable influence on the stability of Ga-68-labeled FSC conjugates.

In Vitro Characterization

All three Ga-68-labeled FSC-RGD conjugates showed hydrophilic properties following the order of [68Ga]FSC(RGDfE)3 (−3.8 ± 0.2) > [68Ga]FSC(succ-RGD)3 (−3.6 ± 0.1) > [68Ga]FSC(Mal-RGD)3 (−3.4 ± 0.0).

Binding of [125I]c(RGDyV to integrin αvβ3 was successfully displaced by all FSC-RGD conjugates and c(RGDyV) in a concentration-dependent manner. IC50 values were 1.8 ± 0.7 nM for FSC(succ-RGD)3, 2.1 ± 0.9 nM for FSC(RGDfE)3, and 3.4 ± 0.6 nM for FSC(Mal-RGD)3, indicating enhanced binding affinities as compared to c(RGDyV) (6.2 ± 1.6 nM).

The internalization ability of Ga-68-labeled FSC-RGD conjugates is shown in Fig. 1. The internalized activities were 5.7 ± 0.6 % for [68Ga]FSC(succ-RGD)3, 5.3 ± 0.7 % for [68Ga]FSC(RGDfE)3, and 3.0 ± 0.0 % for [68Ga]FSC(Mal-RGD)3 of total activity per milligram protein (% cpm/mg) after 90-min incubation. The corresponding activities were reduced to 0.2 to 0.4 % cpm/mg of the reference activity via addition of excess of c(RGDyV) which demonstrated receptor-specific internalization.

Fig. 1

Internalization of [68Ga]FSC(succ-RGD)3, [68Ga]FSC(RGDfE)3, and [68Ga]FSC(Mal-RGD)3 in integrin αvβ3-positive M21 tumor cells.

The data for the biodistribution studies of all three Ga-68-labeled FSC-RGD conjugates in BALB/c nude mice bearing both integrin αvβ3-positive (M21) as well as integrin αvβ3-negative (M21-L) human melanoma tumors 1 h p.i. are presented in Table 1 and the tumor to tissue ratios in Fig. 2. The activity accumulation in the M21 tumor for the three compounds is decreasing in the order: [68Ga]FSC(RGDfE)3 (5.49 ± 0.94 %ID/g) > [68Ga]FSC(succ-RGD)3 (3.69 ± 0.94 %ID/g) > [68Ga]FSC(Mal-RGD)3 (2.62 ± 0.27 %ID/g). The receptor-specific uptake is demonstrated by the lower uptake found in the receptor-negative M21-L tumor (1.10 ± 0.30, 1.25 ± 0.06, 0.68 ± 0.09 %ID/g, respectively) resulting in comparable M21/M21-L ratios for all three compounds.

Table 1

Biodistribution of [68Ga]FSC(succ-RGD)3, [68Ga]FSC(RGDfE)3, and [68Ga]FSC(Mal-RGD)3 at 1 h p.i. in BALB/c nude mice bearing integrin αvβ3-positive tumors (M-21) on the right flank and integrin αvβ3-negative tumors (M21-L) on the left flank

Organ/tissue	[68Ga]FSC(succ-RGD)3 (% ID/g)	[68Ga]FSC(RGDfE)3 (% ID/g)	[68Ga]FSC(Mal-RGD)3 (% ID/g)
Blood	0.63 ± 0.26	0.40 ± 0.08	0.36 ± 0.08
Spleen	3.27 ± 0.64	9.13 ± 0.27	3.48 ± 0.56
Pancreas	0.61 ± 0.13	1.04 ± 0.12	0.46 ± 0.07
Stomach	2.02 ± 1.35	4.76 ± 0.25	2.24 ± 0.17
Intestine	2.41 ± 0.80	3.21 ± 0.48	1.61 ± 0.30
Kidneys	8.12 ± 1.09	11.52 ± 1.87	5.77 ± 0.89
Liver	3.54 ± 0.63	12.09 ± 1.34	3.77 ± 0.95
Heart	1.21 ± 0.28	1.52 ± 0.13	0.70 ± 0.05
Lung	2.42 ± 0.22	2.48 ± 1.07	1.42 ± 0.26
Muscle	0.52 ± 0.19	0.94 ± 0.09	0.37 ± 0.08
M21	3.69 ± 0.94	5.49 ± 0.94	2.62 ± 0.27
M21-L	1.10 ± 0.30	1.25 ± 0.06	0.68 ± 0.09

Each data point represents an average of three to four animals

Fig. 2

Comparison of M21 melanoma to tissue ratios of [68Ga]FSC(succ-RGD)3, [68Ga]FSC(RGDfE)3, and [68Ga]FSC(Mal-RGD)3 at 1 h p.i. M21/M21-L human melanoma xenografted nude mice were used. Significant differences in uptake are marked with an asterisk (P < 0.05).

A statistical significant difference in the biodistribution data of the three radioligands was observed only for spleen and liver. [68Ga]FSC(succ-RGD)3 showed superior tumor to tissue ratios in aforementioned organs compared to the other two radioligands.

MicroPET/CT Studies

MicroPET/CT studies with BALB/c nude mice bearing αvβ3-positive tumors were performed in order to compare the imaging properties and the in vivo pharmacokinetics of [68Ga]FSC(succ-RGD)3, [68Ga]FSC(RGDfE)3, and [68Ga]FSC(Mal-RGD)3. All three radioligands showed receptor-specific uptake accompanied by predominantly renal elimination at 1 h p.i., resulting in good image contrasts (Fig. 3). In the static image of [68Ga]FSC(succ-RGD)3, the αvβ3-positive tumor is clearly visualized with high resolution whereas unspecific uptake of the radioligand is minimal with the exception of the kidneys. To further evaluate the imaging properties of [68Ga]FSC(succ-RGD)3, dynamic PET imaging was performed and the time-activity curves of tumor, kidney, and heart were extracted (Fig. 4). The dynamic images allow visualization of the receptor-positive tumor as early as 10 min p.i., confirming the rapid accumulation of [68Ga]FSC(succ-RGD)3 in the tumor. The time-activity curves of the kidneys and heart from dynamic PET data showed rapid clearance of [68Ga]FSC(succ-RGD)3 from the circulation while the time-activity curve of the tumor showed a clear tracer retention. To directly compare the imaging properties of [68Ga]FSC(succ-RGD)3 and [68Ga]NODAGA-RGD radiotracers, static (Fig. 5a) and dynamic PET (Fig. 5b, c) imaging using mice bearing U87MG xenograft tumors was carried out with both radiotracers. Three-dimensional volume projections of fused microPET/CT static images for [68Ga]FSC(succ-RGD)3 and [68Ga]NODAGA-RGD were carried out at 90 min p.i. by two mice imaged per day on two consecutive days where on day 1, mouse 1 received tracer A and mouse 2 tracer B and vice versa. The dynamic microPET studies were carried out in the same mouse by 5 min PET scan per frame over 90 min p.i. Both static and dynamic PET images showed uptake in U87MG tumors of both radiotracers, however, with improved tumor delineation for [68Ga]FSC(succ-RGD)3. From the quantitative region of interest (ROI) analysis, uptake values of [68Ga]FSC(succ-RGD)3 in tumor, kidneys, and muscle were 3.8, 3.0, and 0.78 %ID/g at 90 min p.i., while the corresponding data for [68Ga]NODAGA-RGD was 1.6, 1.0, and 0.32 %ID/g, respectively. Despite an approximately 3-fold higher tumor uptake, tumor to muscle (4.9 vs. 5) and tumor to kidney ratios (1.3 vs. 1.6) are comparable.

Fig. 3

Three-dimensional volume projections of fused microPET/CT static images of a nude mouse bearing a M21 xenograft tumor at 1 h p.i. a [68Ga]FSC(succ-RGD)3, b [68Ga]FSC(RGDfE)3, and c [68Ga]FSC(Mal-RGD)3. Red arrow: integrin αvβ3-positive M21 tumor. Injected dose per mouse 5 MBq.

Fig. 4

a Dynamic PET imaging of [68Ga]FSC(succ-RGD)3 in a nude mouse bearing a M21 tumor xenograft. Injected dose 5 MBq. Red arrow: integrin αvβ3-positive M21 tumor. b The dynamic clearance curves of [68Ga]FSC(succ-RGD)3 in selective tissues over 45 min.

Fig. 5

a Three-dimensional volume rendered projections of fused microPET/CT static images for [68Ga]FSC(succ-RGD)3 and [68Ga]NODAGA-RGD at 90 min p.i. (two mice imaged per day on two consecutive days where on day 1, mouse 1 received tracer A and mouse 2 tracer B and vice versa)). b Dynamic PET images of [68Ga]FSC(succ-RGD)3 and c [68Ga]NODAGA-RGD in the same mouse on two consecutive days. Scan duration 5-min PET scan per frame (18 frames). d Quantitative ROI analysis of uptake of [68Ga]FSC(succ-RGD)3 and [68Ga]NODAGA-RGD in tumor, kidneys, and muscle of the same BALB/c mice for 90 min p.i. on two consecutive days. Mice bearing U87MG xenograft tumors; injected dose 6 MBq.

Discussion

Many radiolabeled cyclic RGD peptides have been evaluated as SPECT and PET radiotracers for imaging integrin αvβ3 expression. Among these tracers, radiolabeled multivalent RGD peptides, mainly dimeric and tetrameric derivatives, have been studied extensively on the basis of the multivalency concept [6, 20]. These multimeric RGD peptides exhibited improved receptor affinity due to the avidity effect or simultaneous multivalent binding and prolonged target retention due to increased tracer concentration compared to that of their monomeric analogues. However, comparison of dimeric and tetrameric cyclic RGD peptides showed superiority of dimers over tetramers with respect to tumor to tissue ratios [20]. The longer retention in nontarget tissues, mainly due to higher molecular weight, results in slower elimination which could not be compensated for by the higher tumor uptake of tetrameric constructs. Recently, TRAP(RGD)3 was reported as a trimeric RGD peptide for 68Ga labeling and showed comparable tissue uptake to monomeric analogues but significant enhanced tumor uptake providing the potential for imaging of low-level integrin expression in tissues [13]. Based on these findings, great attention should be taken to reach a subtle balance between the tumor uptake and tumor to tissue ratios.

Recently, we reported three FSC-based trimeric RGD conjugates [16] labeled with Zr-89 showing excellent in vitro stability. PET imaging of [89Zr]FSC(succ-RGD)3 in BALB/c nude mice demonstrated receptor specificity of FSC-RGD conjugates with high accumulation in αvβ3-positive tumors whereas αvβ3-negative tumors were not visualized during the 24 h monitoring period. To further investigate these promising properties of these FSC-RGD conjugates, we now describe the characterization and, in particular, studies on the imaging properties of Ga-68-labeled FSC-RGD conjugates in two tumor models including static and dynamic imaging.

In the present study, all three FSC-RGD conjugates, namely FSC(succ-RGD)3, FSC(RGDfE)3, and FSC(Mal-RGD)3, were successfully labeled with Ga-68 following the protocol that we reported previously [15]. Quantitative labeling of FSC-RGD conjugates was performed at pH 4.5 at RT within 10 min. The logD values of three Ga-68-labeled FSC conjugates ranged from −3.4 to −3.8, displaying a more hydrophilic character compared to their Zr-89-labeled counterparts which ranged from −2.9 to −3.0 [16]. The difference of lipophilicity may result from the different net charges of the radiolabeled compounds (the net charge of [68Ga3+]FSC chelate itself is 0 while that of [89Zr4+]FSC chelate is +1).

Competition studies demonstrated the enhanced binding affinity of the multimeric FSC-RGD conjugates compared with the monomeric c(RGDyV), with highest affinities for FSC(succ-RGD)3 and FSC(RGDfE)3. This was further confirmed by internalization assays with the Ga-68-labeled FSC-RGD conjugates which result in much higher internalization compared to [68Ga]NODAGA-RGD. The differences in binding affinity and internalization properties between the different conjugates can be attributed to the influence of the different linkers (e.g., length and hydrophilicity), whereby FSC(Mal-RGD)3 with the longest linker showed the lowest affinity and lowest internalization values, whereas FSC(succ-RGD)3 and FSC(RGDfE)3 were comparable. Compared with Zr-89-labeled FSC-RGD conjugates [16], the same trend of internalization is confirmed even though the Zr-89-labeled compounds showed slightly lower internalization values than their Ga-68 counterparts.

The biodistribution data of [68Ga]FSC(succ-RGD)3, [68Ga]FSC(RGDfE)3, and [68Ga]FSC(Mal-RGD)3 in BALB/c nude mice bearing integrin αvβ3-positive M21 tumors at 1 h p.i. were directly compared. All three compounds exhibited target-specific binding with enhanced tumor uptakes compared to [68Ga]NODAGA-RGD (1.3 %ID/g [14]) and relative low uptakes in nontarget tissue. PET studies revealed high-contrast images of the αvβ3-positive M21 tumor at 1 h, confirming the biodistribution data (Table 1 and Fig. 3). Among the three compounds, [68Ga]FSC(succ-RGD)3 showed superior tumor to tissue ratios for spleen and liver, which is the reason that [68Ga]FSC(succ-RGD)3 was chosen for further studies. Comparing the tumor to tissue ratios of [68Ga]FSC(succ-RGD)3 at 1 and 2 h p.i. (Fig. S1), increased tumor to background ratios were found for the later time point providing the potential for delayed imaging.

Biodistribution and tumor targeting of [68Ga]FSC(succ-RGD)3 were very comparable to its Zr-89 counterpart [16]. Tumor and organ uptake values at 1 h p.i. were not significantly different, an exception was a significantly higher activity of the [68Ga]FSC-RGD conjugate in blood, liver, spleen, and αvβ3-negative M21-L tumor, the later tissues, however, minor in terms of absolute values. This could be explained by a different biological behavior and binding of released Ga-68 by transferrin resulting in longer blood circulation. On the other hand, no indication of differences in in vitro stability or protein binding of the complexes was found and image contrast in microPET images was excellent. Therefore, these differences could also be related to the different net charges of the FSC chelate.

In Table 2, tumor to tissue ratios of [68Ga]FSC(succ-RGD)3 are compared with the literature data of [68Ga]TRAP(RGD)3 and [68Ga]NODAGA-RGD. Overall, very similar ratios are observed for [68Ga]FSC(succ-RGD)3 and [68Ga]TRAP(RGD)3 except for the tumor to blood ratio. [68Ga]TRAP(RGD)3 exhibited higher ratios than [68Ga]FSC(succ-RGD)3 at 1 and 2 h p.i., which is probably due to a faster clearance from blood of [68Ga]TRAP(RGD)3. Notably, the tumor to kidney ratios of [68Ga]FSC(succ-RGD)3 and [68Ga]TRAP(RGD)3 are almost the same, indicating that the relative high kidney excretion is mainly determined by the multimeric RGD peptide part and not the chelator moiety. However, whereas for [68Ga]TRAP(RGD)3, tumor to background ratios remained constant over time, for our compound, tumor to background ratios improved up to 2 h p.i. again indicating an advantage of PET imaging at late time points for [68Ga]FSC(succ-RGD)3. In particular, much higher tumor to muscle ratios were observed (14.4 vs. 6.9 for [68Ga]TRAP(RGD)3). Compared with the data found for [68Ga]NODAGA-RGD, [68Ga]FSC(succ-RGD)3 exhibited different tumor to tissue ratios for blood and kidney. Even though not statistically significant, [68Ga]NODAGA-RGD exhibited 1.8-fold higher tumor to blood and 2-fold higher tumor to kidney ratios 1 h p.i. These differences could be attributed to a slower blood clearance rate and kidney excretion of [68Ga]FSC(succ-RGD)3. However, they were not confirmed in PET imaging, where comparable tumor to tissue ratios were found. The direct comparison of [68Ga]FSC(succ-RGD)3 with [68Ga]NODAGA-RGD in mice bearing U87MG xenograft tumors by static and dynamic PET imaging (Fig. 5) demonstrated receptor-specific binding for both compounds. Both Figs. 4 and 5d show not only enhanced tumor accumulation (3.8 vs. 1.6 %ID/g, 90 min p.i.) but also high retention of [68Ga]FSC(succ-RGD)3 in the receptor-positive tumors during the observation period, which is quite similar to the reported [68Ga]TRAP(RGD)3. In contrast, washout of [68Ga]NODAGA-RGD from U87MG xenografts was considerably faster, as can be seen in the dynamic PET images. Whereas for [68Ga]FSC(succ-RGD)3, no significant loss of image contrast even at 90 min p.i. was found, [68Ga]NODAGA-RGD exhibited significant decrease from 35 min p.i. onward.

Table 2

Comparison of M21 to tissue ratios of [68Ga]FSC(succ-RGD)3 with literature data for [68Ga]TRAP(RGD)3 [13] and [68Ga]NODAGA-RGD

	[68Ga]FSC(succ-RGD)3	[68Ga]FSC(succ-RGD)3	[68Ga]TRAP(RGD)3	[68Ga]TRAP(RGD)3	[68Ga]NODAGA-RGD
M21/tissue	1 h	2 h	1 h	2 h	1 h
M21/blood	6.4 ± 2.5	18.7 ± 2.7	19.4 ± 9.1	28.4 ± 19.6	11.3 ± 6.6
M21/spleen	1.1 ± 0.2	1.1 ± 0.1	1.8 ± 0.7	1.3 ± 0.7	0.9 ± 0.4
M21/pancreas	6.0 ± 0.4	10.7 ± 0.8	6.9 ± 1.9	5.7 ± 2.6	6.1 ± 3.1
M21/stomach	1.8 ± 1.3	1.8 ± 0.9	1.4 ± 0.6	1.3 ± 0.8	1.7 ± 0.7
M21/intestine	1.6 ± 0.4	1.9 ± 0.6			1.5 ± 0.7
M21/kidneys	0.5 ± 0.1	0.6 ± 0.1	0.6 ± 0.2	0.5 ± 0.3	1.0 ± 0.4
M21/liver	1.0 ± 0.2	1.4 ± 0.2	1.2 ± 0.5	1.2 ± 0.7	0.8 ± 0.3
M21/heart	3.1 ± 0.8	6.2 ± 0.6	4.7 ± 2.4	3.2 ± 2.7	5.9 ± 2.4
M21/lung	1.5 ± 0.3	2.1 ± 0.1	2.1 ± 0.9	2.2 ± 1.3
M21/muscle	7.3 ± 0.8	14.4 ± 3.3	6.4 ± 1.9	6.9 ± 3.7	6.1 ± 3.5
M21/M21-L	3.4 ± 0.9	4.3 ± 2.2	4.1 ± 1.4	2.7 ± 1.6	4.0 ± 2.3

The same murine mouse model was used for all compounds. M21 to tissue ratios of [68Ga]NODAGA-RGD were calculated based on the literature data [14]

The enhanced tumor accumulation in addition to the good tumor retention for [68Ga]FSC(succ-RGD)3 not only allows PET imaging at late time points, but also provides the possibility to achieve the same contrast using less radioactivity, which is expected to reduce the radiation burden. Moreover, it is of interest for small animal imaging where the same image quality can be achieved with less radioactivity injected.

Taking all these into account, [68Ga]FSC(succ-RGD)3 has several advantages compared to [68Ga]NODAGA-RGD and possibly to other monomeric RGD peptides. First, the improved tumor accumulation allows for delayed imaging with potentially improved image contrast; second, it provides the potential to use lower activity to reach the same image contrast; third, the high affinity of [68Ga]FSC(succ-RGD)3 provides the potential for imaging of low-level integrin expression in tissues as Notni et al. mentioned [13].

Conclusion

Three trimeric FSC-RGD conjugates were quantitatively labeled with Ga-68 within 10 min at RT. The Ga-68-labeled compounds showed high stability in challenging solutions and hydrophilic behavior. In vitro and in vivo studies including PET/CT imaging demonstrated their high affinity for the integrin αvβ3, receptor-selective tumor uptake, rapid predominantly renal excretion, and excellent imaging properties. The comparison of [68Ga]FSC(succ-RGD)3 and [68Ga]NODAGA-RGD shows the advantages of [68Ga]FSC(succ-RGD)3 in respect of the possibility to carry out delayed imaging with improved tumor to background ratios, imaging with reduced radiation dose, and higher binding affinity allowing monitoring of low-level integrin expression in tissues.

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