Abstract
Radiohalogenated agents are often the first line of pursuit in the development of new radiopharmaceuticals—whether antibodies, peptides, or small molecules—because of their ease of synthesis, lack of substantial steric perturbation of the original affinity agent (in some cases, providing enhanced affinity), and capacity to be transformed into therapeutics (in some cases, with a mere switch of an isotope). They often provide proof of a principle before optimization for pharmacokinetics or generation of radiometallated agents, when the latter are necessary. In particular, 18F has been well integrated into normal clinical work flow in the form of 18F-FDG for oncologic imaging, with reliable daily production and distribution to sites for immediate use, without the need for on-site preparation. Here we discuss radiohalogenated versions of imaging and therapeutic agents targeting the prostate-specific membrane antigen (PSMA); these were among the first such agents to be synthesized and used clinically. PSMA is highly expressed on prostate cancer epithelial cells and is currently being extensively investigated around the world as a target for imaging and therapy of prostate cancer. Additionally, the presence of PSMA on nonprostate tumor neovasculature has opened the possibility of PSMA-targeted molecules as generalizable cancer imaging and therapy agents. We focus on 18F-labeled agents for PET, as they begin to redefine—along with the corresponding 68Ga-labeled agents discussed elsewhere in this supplement to The Journal of Nuclear Medicine—the management of prostate cancer across a variety of clinical contexts.
Prostate cancer (PC) is the most common noncutaneous malignancy in men (1). Initial suspicion often results from elevated levels of prostate-specific antigen (PSA) in serum. The workup at diagnosis involves physical examination and often proceeds to biopsy to validate the presence of cancer. For further staging, restaging, and diagnosis of recurrence, as well as for therapeutic monitoring, noninvasive imaging tests may be incorporated. The most widely accepted imaging modalities used include MRI for the evaluation of patients who have clinically localized primary disease (2) or who are thought to harbor recurrent PC limited to the pelvis (3), contrast-enhanced CT, and 99mTc-methylene diphosphonate bone scanning for the evaluation of metastatic disease in primary and recurrent PC (4). Additionally, in Europe, PET imaging with 11C-choline or 18F-fluorocholine has recently gained acceptance for the workup of recurrent PC.
However, those modalities possess significant limitations (5,6). Conventional imaging has not adequately addressed a variety of important clinical issues, including pretherapy risk stratification, reliable pretherapy staging of patients at risk for pelvic lymph node metastases or systemic disease, and the detection of biochemical recurrence at low PSA levels in patients previously treated for PC with curative intent. In the context of such limitations, several agents for the molecular imaging of PC have been developed. These include radiotracers that target lipid metabolism (7), function as nucleoside analogs (8), and bind with high affinity to PC-specific molecular targets, such as the androgen receptor (9), bombesin receptor (10,11), and prostate-specific membrane antigen (PSMA) (12,13). PSMA is a particularly promising target in light of its nearly universal expression in PC and the correlation of increased PSMA expression with tumor aggressiveness (14–16). These various molecular agents may provide the improved imaging reliability necessary to address the shortcomings of conventional imaging currently used to guide PC therapy.
The first PSMA-targeted imaging agent to gain transient clinical acceptance was 111In-capromab pendetide (ProstaScint; Aytu BioScience, Inc.), a monoclonal antibody against an intracellular epitope of PSMA (17). Ultimately, the targeting of an intracellular epitope combined with the limitations in spatial resolution and quantification that are inherent to single-photon–emitting radionuclides prevented the acquisition of suitably high-quality images. However, PSMA remained a promising target, and more recent radiolabeled monoclonal antibodies against an extracellular PSMA epitope (18,19) as well as single-photon–emitting (20,21) and positron-emitting (22–25) small-molecule inhibitors of PSMA have been extensively explored. Results continue to suggest that PSMA-targeted imaging of PC is a promising alternative to conventional imaging.
The preliminary success of [177Lu-DOTA0,Tyr3]octreotate (26) as a therapeutic agent provided a strong rationale for extending small-molecule, targeted radiopharmaceutical therapy (RPT) to PC. As discussed elsewhere in this supplement, RPT with PSMA-targeted agents is beginning to proliferate in Europe, along with application of the β-particle emitter 177Lu (27,28). Isotopic analogs of some of the radiohalogenated imaging agents mentioned earlier may also be used for therapy. Accordingly, radiohalogenated agents targeting PSMA may serve as effective theranostic agents in the future.
Here we review the available literature on the preclinical and clinical development of radiohalogenated small-molecule inhibitors of PSMA, with particular emphasis on 18F-labeled agents applicable to PET. We also briefly review the potential of α-particle–emitting and Auger electron–emitting radiohalogenated agents for RPT.
RADIOHALOGENATED INHIBITORS OF PSMA AS IMAGING AGENTS
Several scaffolds have been used in the synthesis of small-molecule PSMA inhibitors; these include thiols, carbamates, phosphoramidates, phosphinic acids, and ureas (29–33)—the latter two structural categories having been administered to human subjects. A urea-based molecule (11C-MCG or 11C-DCMC) was the first reported preclinical PET agent for PSMA-targeted imaging (Fig. 1) (34). Soon after, the first radiohalogenated small-molecule inhibitor of PSMA (125I-DCIT) was reported (Table 1; Fig. 1) (35). Both of those early examples of PSMA-targeted small molecules demonstrated uptake in PSMA-expressing PC xenografts derived from a lymph node metastasis, but neither was labeled with an ideal radionuclide for human applications.
Chemical structures of small-molecule inhibitors of PSMA.
Selected Characteristics of Radiohalogenated PSMA-Targeted Agents
Although neither 11C-DCMC nor 125I-DCIT was investigated in human trials, each showed that in vivo imaging of PSMA was possible in preclinical models. Later-generation radioiodinated agents developed for SPECT and PET (124I) as well as for β-particle therapy were used in clinical trials (20,36,37). A radiofluorinated small-molecule inhibitor (18F-DCFBC) (Table 1; Fig. 1) was synthesized and found to accumulate in PSMA-positive PC xenografts (38), suggesting an 18F-labeled derivative for translation. As discussed in greater detail later in this review, several considerations are important in choosing a specific radionuclide for PET imaging; 18F is the superior choice for imaging today in the United States. Although much of the early clinical literature on PSMA-targeted imaging with small molecules focused on agents labeled with the radiometal 68Ga (24,39), a series of small but informative prospective studies have now been performed with 18F-DCFBC (22,40,41). A higher-affinity and more easily synthesized 18F-labeled small molecule for PET imaging of PSMA (18F-DCFPyL) (Table 1; Fig. 1) (42) was subsequently tested in preclinical models and found to have higher uptake than 18F-DCFBC in PSMA-expressing PC xenografts (38).
Additional 18F-labeled small molecules that do not contain a urea moiety have also been reported. For example, the phosphonomethyl-based small molecule BAY 1075553 (Table 1; Fig. 1) was investigated in both preclinical models (43) and a first-in-man trial that showed safety and efficacy (44).
Recently, Yang et al. reported preclinical results obtained with a series of carbamates that shared structural similarities with the urea-based PSMA inhibitors (30). Those agents, including 4-bromo-2-18F-fluorobenzoyllysineoxypentanedioic acid (4-bromo-2-18F-fluorobenzoyllysine OPA) and 4-iodo-2-18F-fluorobenzoyllysineoxypentanedioic acid (4-iodo-2-18F-fluorobenzoyllysine OPA) (Table 1; Fig. 1), showed high tumor uptake and low nontarget tissue retention in preclinical studies. These results suggested that the use of carbamates may be an approach for mitigating toxicity in endoradiotherapeutic applications.
PSMA-TARGETED IMAGING: IMPLICATIONS FOR MANAGING PC
The potential applications of PSMA-targeted imaging of PC are manifold. PC is often initially diagnosed because of elevated levels of PSA in serum. However, histologic proof of a tumor by biopsy is required for definitive diagnosis (45). Not infrequently, biopsy does not succeed in demonstrating a tumor on the first attempt and may need to be repeated, placing the patient at risk for complications (46). Furthermore, therapeutic decisions, ranging from active surveillance to systemic therapy, are made on the basis of the grade and stage of a tumor (45). However, the performance of imaging procedures currently in use, such as MRI, CT, and bone scanning, has not been satisfactory with regard to the staging of disease (5,6). This issue may lead to a significant proportion of patients being either under- or overtreated. Furthermore, biochemical (PSA) relapse is observed in about 30% of patients undergoing treatment with curative intent (47). In cases of biochemical recurrence after radical prostatectomy, salvage radiation therapy of the prostatic fossa is often recommended (45) and performed without proof of the location of recurrent tumor tissue exclusively within the intended field of radiation.
The accumulation of clinical data obtained with PSMA-targeted PET imaging agents has suggested that some of the limitations of conventional imaging may be addressed by this new modality. Such an approach may allow for more individually tailored therapy with regard to selective surgery or radiation therapy or for the selection of patients for new therapeutic options (such as PSMA-based RPT (28)). A growing number of studies, mainly with 68Ga-labeled PSMA radiotracers, have provided promising results with regard to the clinical utility of PSMA-targeted imaging (24,39,48). In Europe, 68Ga-PSMA PET imaging has already been integrated into the routine diagnostic workup of PC at selected centers. The rising demand for PSMA-targeted imaging justifies the implementation of 18F-labeled radiotracers for such imaging. Practical considerations regarding 18F versus 68Ga are discussed later in this review (22,23,44,49).
The first-in-man experience with 18F-DCFBC was described by Cho et al. (22). The biodistribution of the radiotracer in human subjects included high uptake in the kidneys. The primary route of excretion of 18F-DCFBC was renal, with the bladder wall having a higher absorbed dose than any other organ. One potential limitation that was apparent with 18F-DCFBC was the persistently high blood-pool activity even 2 h after radiotracer administration. Nonetheless, 18F-DCFBC uptake was seen in all sites of lymph node and bone metastatic PC that were apparent on conventional imaging with CT and bone scanning as well as in multiple sites that were suspected of having early metastatic disease but that were occult on other types of imaging. Those results implied that PSMA-targeted imaging could have an improved ability to stage patients before local therapy and might also yield more satisfactory identification of sites of disease in patients with biochemical recurrence.
A follow-up prospective study investigating the utility of 18F-DCFBC in primary PC was recently published (40). In that study, 13 patients were imaged with 18F-DCFBC PET/CT, and 12 also underwent prostate MRI before radical prostatectomy. Although MRI appeared to be more sensitive for the detection of PC in this small series, 18F-DCFBC PET/CT had a high specificity for the identification of aggressive PC and also showed no evidence of uptake in benign prostatic hyperplasia. A positive correlation between the Gleason score and 18F-DCFBC uptake was found, although the small sample size made it difficult to ascertain the strength of the correlation and the authors reported a wide confidence interval associated with this finding (ρ, 0.65; 95% confidence interval, 0.16–0.89). If such a correlation could be confirmed in larger prospective trials, then PSMA PET might prove to be a noninvasive means of risk stratification for patients with PC.
In a separate prospective trial of 17 patients with known progressive, metastatic PC, Rowe et al. reported that 18F-DCFBC PET/CT was more sensitive than the conventional imaging modalities of CT and bone scanning for the detection of suspect lesions (592 positive lesions, along with an additional 63 equivocal lesions, with 18F-DCFBC PET/CT; 520 positive lesions, along with 61 equivocal lesions, with CT and bone scanning) (41). The superior detection by 18F-DCFBC was found in patients with both hormone-naïve and castration-resistant PC and was seen with lymph node, bone, and visceral lesions. Again, these findings suggested the potential utility of PSMA-targeted imaging for staging before therapy and for the detection of biochemically recurrent PC.
Chen et al. published promising preclinical data on 18F-DCFPyL, a PSMA-selective ligand with high binding affinity (42). More recently, Szabo et al. published first-in-man data demonstrating that this radiotracer was safe and showed the expected biodistribution (23). Dietlein et al. reported the first clinical experience in a series of patients examined with both 18F-DCFPyL PET/CT and 68Ga-PSMA PET/CT (49). In that study, the number and the SUVmax of PSMA-positive lesions detected by the radiotracers were compared in 14 patients with recurrent PC. In addition to detecting lesions identified by 68Ga-PSMA, 18F-DCFPyL PET/CT imaging detected additional lesions in 3 patients (Fig. 2). The authors concluded that 18F-DCFPyL PET/CT provides high image quality and compares favorably with 68Ga-PSMA PET/CT, particularly with regard to the sensitive detection of small lesions.
Predominantly lytic bone metastasis (arrow) (A) that was occult on 68Ga-PSMA PET (B) and PET/CT (C) but readily apparent on 18F-DCFPyL PET (D) and PET/CT (E).
Since the publication of the study of Dietlein et al. (49), 18F-DCFPyL imaging has been systematically offered for clinical purposes by the same group. To date, 139 patients have been examined with 18F-DCFPyL for a variety of diagnostic purposes; however, patients were referred predominantly for localization after biochemical recurrence (unpublished data). Other indications have included staging at primary diagnosis, restaging, therapy planning and disease monitoring in cases of castration resistance, and selection for 177Lu-PSMA RPT. 18F-DCFPyL has proven to be of high value for detecting local recurrences and lymph node and bone metastases, even at very low PSA levels (<0.5 ng/dL) (Fig. 3). A systematic, retrospective evaluation of the collected clinical 18F-DCFPyL PET/CT data (and a comparison group of 68Ga-PSMA data) is under way and will be published elsewhere.
Detection of wide variety of PC lesions with 18F-DCFPyL. Locally recurrent PC (CT [A] and 18F-DCFPyL PET/CT [B]) and lymph node (CT [C] and 18F-DCFPyL PET/CT [D]) and bone (CT [E] and 18F-DCFPyL PET/CT [F]) lesions were visible as marked focal radiotracer uptake (arrows).
18F VERSUS 68Ga: PRACTICAL CONSIDERATIONS
At present, for PSMA-targeted PET imaging, 68Ga-labeled radiotracers are most commonly used. A major advantage of 68Ga labeling is the commercial availability of germanium/gallium generators. The availability of such generators allows on-site synthesis of 68Ga-labeled PET radiotracers at centers without access to a cyclotron and with only a modest investment in infrastructure dedicated to radiopharmaceutical synthesis. 18F labeling requires access to a cyclotron but has several distinct advantages. Generally, the higher production capability allows the synthesis of larger batches, allowing many examinations to be performed in sequence on the basis of a single synthesis. A single 68Ga-based synthesis will usually enable the production of a sufficient amount of radiotracer for only 3 or 4 examinations. Additionally, the longer physical half-life of 18F (109 min) than of 68Ga (68 min) allows for easier transportation of the radiotracer from central production sites to remote imaging centers, obviating the need for on-site radiosynthesis personnel.
At present, the production of 18F-DCFPyL can be performed in 2 steps. The first step consists of the preparation of an activated ester (2,3,5,6-tetrafluorophenyl 6-18F-fluoronicotinate), which is subsequently coupled to the (S)Lys-C(O)-(S)Glu motif. The final product, 18F-DCFPyL, is then purified by preparative high-performance liquid chromatography. A purification method based on solid-phase extraction is in development. Translation of this radiosynthesis method to commercially available synthesis modules with disposable cassettes is imminent (personal communication). The expense for the synthesis of 18F-DCFPyL with an automated system is expected to be similar to that for the synthesis of 68Ga-PSMA. Consequently, 18F-DCFPyL could be produced in larger amounts than its 68Ga-labeled analog and at a similar expense.
Differences in image quality may represent another important factor supporting the adoption of 18F-labeled PSMA-targeted radiotracers. As a result of favorable dosimetry, the injection of higher radiotracer doses leads to improved image statistics. 68Ga also has a lower positron yield (89.14%; that for 18F is 96.86% (50)) and exhibits several single-photon emissions, resulting in an increase in image noise. Compensating by increasing the scan time for the injected dose is difficult because of the shorter half-life of 68Ga. A further advantage of 18F is that its spatial resolution is higher than that of 68Ga because of its lower positron energy (1,899 keV for 68Ga vs. 633 keV for 18F). In the case of lower kinetic energy, the locations of the positron emission and the annihilation point are closer, resulting in better resolution of PET images. Accordingly, higher intrinsic image resolution for 18F-labeled radiotracers is possible.
RADIOHALOGENATED PSMA-TARGETED SMALL MOLECULES FOR THERAPY
A key aspect of targeted RPT is selecting a radionuclide with characteristics that balance minimum toxicity to normal tissues and maximum efficacy for a particular clinical application. Because the clinical evaluation of novel cancer therapeutics is generally initiated in patients with advanced disease, PSMA-targeted RPT was first evaluated with β-emitters whose longer range should have been advantageous in that setting. The targeting potential of a series of radioiodinated PSMA inhibitors was demonstrated by Hillier et al. (51) and formed the basis for the clinical evaluation of 131I-MIP-1095 in 28 patients with metastatic castration-resistant PC (37). However, as discussed elsewhere in this supplement, most current work with β-emitters for PSMA-targeted RPT is focused on radiometals such as 177Lu because of perceived advantages in emission spectra and convenience.
Perhaps the most important potential application of PSMA-targeted RPT is the treatment of micrometastatic disease. In that setting, it is essential to be able to deliver tumoricidal doses of radiation to small clusters of malignant cells while sparing neighboring normal tissues. Two types of radiation—Auger electrons and α-particles—have a higher potency and a shorter tissue range than β-particles; these characteristics should make them suitable for the treatment of microscopic disease (52). The linear energy transfers of Auger electrons and α-particles are about 4–26 and 100 keV/μm, respectively (that for most β-emitters is ∼0.2 keV/μm); these values confer a greater deposition of energy within small volumes and a higher cytotoxicity (53). Unlike β-particles, which have path lengths of up to 1,000 cell diameters, the range of α-particles is only about 5–10 cell diameters and the range of most Auger electrons is considerably smaller than 1 cell. The feasibility of treating metastatic PC with an α-emitting radiopharmaceutical was demonstrated in a phase III trial with 223RaCl2 (Alpharadin; Bayer) (54); however, its mechanism of uptake limits its application to bone metastases. Exploiting PSMA as a molecular target offers the exciting prospect of treating micrometastatic disease in both bone and soft tissues.
With regard to Auger electron emitters, Kiess et al. evaluated the therapeutic potential of 125I-DCIBzL (Table 1; Fig. 4) for treating PC (55). 125I has been the prototypical radionuclide for Auger electron therapy experiments because it emits an average of approximately 20 electrons per decay, with a tissue range of less than 0.5 μm, and requires localization of the site of its decay to the cell nucleus for maximum cytotoxicity (56). In cell culture experiments, 125I-DCIBzL treatment resulted in PSMA-specific killing, as evidenced by increased DNA damage and decreased clonogenic survival in PSMA-positive (PC3 PIP) versus PSMA-negative (PC3 flu) cells. Treatment of PC3 PIP tumors with a 111-MBq dose of 125I-DCIBzL resulted in a significant tumor growth delay. Although these results are highly encouraging, 125I may not be the ideal Auger electron emitter for clinical translation, in part because of its 60-d half-life. Two Auger electron emitters that may offer advantages for PSMA-targeted radiotherapy are radiohalogens—123I (13-h half-life) and 77Br (57-h half-life)—and studies evaluating their suitability with appropriately designed PSMA inhibitors are under way.
Auger electron–emitting (125I-DCIBzL) and α-particle–emitting (211At-DCAtBzL) radiohalogenated small-molecule inhibitors of PSMA.
The radiohalogen 211At has particularly favorable characteristics for clinical development, including a 7.2-h half-life, 100% α-particle emission per decay, and the absence of α-particle–emitting daughters, which can lead to excessive radiation doses to normal tissues when released from the parent molecule (52,53). To investigate the therapeutic potential of PSMA-targeted 211At, 211At-DCAtBzL (Table 1; Fig. 4) was synthesized and evaluated in PSMA-positive PC3 PIP and PSMA-negative PC3 flu human prostate carcinoma models (57). A paired-label biodistribution experiment demonstrated that the uptake of 211At-DCAtBzL in the PSMA-positive xenograft was high over a time course relevant to the half-life of 211At and increased with time, reaching a value of 41.5 ± 18.4 (mean ± SD) percentage injected dose/g at 18 h. Except at 18 h, the uptake of the coadministered 131I analog in the PSMA-positive xenograft was significantly higher, by about 25%–33%. That observation, in concert with increased 211At levels in tissues known to accumulate free halides (stomach and thyroid), suggested that some deastatination of 211At-DCAtBzL had occurred. Nonetheless, these results are highly encouraging, particularly for a non–protein-based agent, because—to the best of our knowledge—that uptake is the highest level of sustained tumor uptake that has been reported for a 211At-labeled targeted radiotherapeutic agent (58).
The therapeutic potential of 211At-DCAtBzL was first investigated in subcutaneous xenografts and then in a newly developed micrometastatic PC model (57). Treatment with 211At-DCAtBzL significantly improved survival in the micrometastatic disease model; however, parallel long-term toxicity studies demonstrated that a meaningful therapeutic benefit occurred in a dose range that also resulted in delayed renal toxicity. α-Camera imaging demonstrated selective uptake of 211At in renal proximal tubules, consistent with the presence of PSMA in these tissues (59). Although 211At-DCAtBzL is not suitable for clinical translation, this compound provided valuable confirmation that 211At-labeled PSMA inhibitors with intact tumor-localizing capacity and reasonable in vivo stability can be synthesized.
FUTURE DIRECTIONS FOR PSMA-TARGETED MANAGEMENT OF PC
The rapid adoption in Europe of predominantly 68Ga-labeled compounds for diagnostic imaging and 177Lu-labeled compounds for RPT hints at the possible transformative capacity of these agents. However, the vast majority of the literature on clinical PSMA-targeted imaging and therapy is retrospective, with only a few small prospective studies to date (40,41,60). The most pressing need in the field of PSMA-based management of PC is a commitment to large, multicenter, prospective, well-designed clinical trials that can definitively prove the utility of these agents in specific clinical settings. Further study of PSMA as an imaging biomarker and noninvasive means of determining levels of androgen signaling during therapy and judging the radiographic response to therapy are also of broad interest and should be studied in a prospective, systematic fashion.
In addition to studies evaluating the role of PSMA-targeted imaging agents in the context of defined clinical issues, studies evaluating the global impact on clinical decision making in PC patients should also be done. Such studies might take a form similar to the National Oncologic PET Registry; that is, prescan and postscan evaluations of treatment plans could be used to gauge the impact of imaging findings on patient management.
Increasing numbers of case reports and small series are demonstrating the possible utility of PSMA-targeted imaging in nonprostate cancers. The localization of a radiotracer in those cancers appears to be based on PSMA expression in tumor neovasculature (61). Clear cell renal cell carcinoma (62–64) and cancers of the thyroid (65), breast (66), and colon (67) are among the tumor types reported to have PSMA-targeted radiotracer uptake. With thoughtful, prospective trials to define the clinical utility of PSMA-targeted imaging in these cancers, PSMA-targeted imaging and therapy may prove to have broad implications in the field of oncology. Indeed, diseases such as metastatic clear cell renal cell carcinoma often have a less indolent course than PC, suggesting that the impact of PSMA-targeted imaging may actually be greater in those conditions.
CONCLUSION
With the exquisite specificity and high sensitivity afforded by PSMA PET radiotracers, the hope is that clinicians will increasingly incorporate PSMA-targeted imaging as part of the routine evaluation and management of men with PC. The use of radiohalogens—already proving useful for therapy in the context of recent clinical trials incorporating 131I—is being extended to α-particle emitters, such as 211At, with an attendant focus on micrometastatic disease.
DISCLOSURE
This work was supported in part by NIH CA124675, CA184228, and CA183031. Under a licensing agreement between Progenics and Johns Hopkins University, Martin G. Pomper is entitled to royalties on an invention described in this article. This arrangement has been reviewed and approved by Johns Hopkins University in accordance with its conflict-of-interest policies. No other potential conflict of interest relevant to this article was reported.
- © 2016 by the Society of Nuclear Medicine and Molecular Imaging, Inc.
REFERENCES
- Received for publication March 1, 2016.
- Accepted for publication August 8, 2016.