Albumin-Binding PSMA Ligands: Implications for Expanding the Therapeutic Window

Kelly, James M.; Amor‐Coarasa, Alejandro; Ponnala, Shashikanth; Nikolopoulou, Anastasia; Williams, C. M.; DiMagno, Stephen G.; Babich, John W.

doi:10.2967/jnumed.118.221150

Cited by 54 publications

(76 citation statements)

References 24 publications

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“…The IC 50 of RPS-074 was determined to be 12.0 6 3.4 nM, a value consistent with the reported PSMA affinities of structurally analogous trifunctional ligands such as RPS-072 (16).…”

Section: In Vitro Evaluationsupporting

confidence: 82%

“…With this in mind, we have focused our efforts on maximizing the therapeutic window of these powerful radiopharmaceuticals. Our choice of RPS-074 for preclinical therapy studies follows the identification of the recently reported analog RPS-072 (16), which showed dramatically reduced kidney uptake and substantially increased and prolonged tumor uptake relative to several novel PSMA-targeting ligands, including PSMA-617, RPS-063 (23), CTT1403 (24), PSMA-Alb-02 (19), and PSMA-Alb-56 (25). Although the DOTA-containing RPS-072 also chelates 225 Ac 31 , radiolabeling yield was only 49%, and the 225 Ac-DOTA complex has been found to have suboptimal in vivo stability (26,27).…”

Section: Discussionmentioning

confidence: 99%

“…Briefly, RPS-074 was generated from the coupling of di-tert-butyl (((S)-1-(tert-butoxy)-6-(3-(3-ethynylphenyl)ureido)-1-oxohexan-2-yl)carbamoyl)-L-glutamate (14), macropa-isothiocyanate (15), and N 6 -(4-(4-iodophenyl)butanoyl)-Llysine by 2 linkers with 3 and 8 PEG units, respectively. RPS-072 was synthesized following a previously published method (16).…”

Section: Chemistrymentioning

confidence: 99%

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A Single Dose of ²²⁵Ac-RPS-074 Induces a Complete Tumor Response in an LNCaP Xenograft Model

et al. 2018

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Promising biochemical responses to 225 Ac-prostate-specific membrane antigen (PSMA) 617, even in patients who are refractory to βparticle radiation, illustrate the potential of targeted α-therapy for the treatment of metastatic castration-resistant prostate cancer. However, side effects such as xerostomia are severe and irreversible. To fully harness the potential of targeted α-therapy, it is necessary to increase the therapeutic index of the targeted radioligands. One emerging strategy is to increase clearance half-life through enhanced binding to serum albumin. We have evaluated the albumin-binding PSMA-targeting ligand RPS-074 in a LNCaP xenograft model to determine its potential value to the treatment of prostate cancer. Methods: 225 Ac-RPS-074 was evaluated in male BALB/c mice bearing LNCaP xenograft tumors. A biodistribution study was performed over 21 d to determine the dosimetry in tumors and normal tissue. The dose response was measured in groups of 7 mice using 37, 74, and 148 kBq of 225 Ac-RPS-074 and compared with positive and negative control groups. Mice were sacrificed when tumor volume exceeded 1,500 mm 3 . Results: 225 Ac-RPS-074 was labeled in greater than 98% radiochemical yield and showed high (.10% injected dose/g) and sustained accumulation in LNCaP tumors from 24 h to beyond 14 d. Signal in blood and highly vascularized tissues was evident over the first 24 h after injection and cleared by 7 d. The tumor-tokidney ratio was 4.3 ± 0.7 at 24 h and 62.2 ± 9.5 at 14 d. A single injection of 148 kBq induced a complete response in 6 of 7 tumors, with no apparent toxic effects. Treatment with 74 kBq induced a partial response in 7 of 7 tumors, but from 42 d, 6 of 7 experienced significant regrowth. The 37-kBq group experienced a survival benefit relative to the negative control but not compared with the positive control group. Conclusion: A single dose of 148 kBq of 225 Ac-RPS-074 induced a complete response in 86% of tumors, with tumor-to-normal-tissue ratios that predict an improved therapeutic index. The use of the macropa chelator enabled quantitative radiolabeling and may facilitate the clinical translation of this promising targeted α-therapeutic. Ac-RPS-074 Induces a Complete Tumor Response in an LNCaP 225 A Single Dose of http://jnm.snmjournals.org/content/60/5/649 This article and updated information are available at: http://jnm.snmjournals.org/site/subscriptions/online.xhtml Information about subscriptions to JNM can be found at: http://jnm.snmjournals.org/site/misc/permission.xhtml

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“…The IC 50 of RPS-074 was determined to be 12.0 6 3.4 nM, a value consistent with the reported PSMA affinities of structurally analogous trifunctional ligands such as RPS-072 (16).…”

Section: In Vitro Evaluationsupporting

confidence: 82%

Section: Discussionmentioning

confidence: 99%

Section: Chemistrymentioning

confidence: 99%

See 1 more Smart Citation

A Single Dose of ²²⁵Ac-RPS-074 Induces a Complete Tumor Response in an LNCaP Xenograft Model

et al. 2018

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“…Serum albumin ( 43 ) functions as a significant regulator of plasma oncotic pressure and a transporter of ligands ( 44 – 46 ). It has a half-life in the body of about 20 days and decreases by 10–15% after 50 years of age ( 47 ).…”

Section: Human Serum Albuminmentioning

confidence: 99%

SARS-CoV-2 Bound Human Serum Albumin and Systemic Septic Shock

Johnson

Fatemi

Winlow

2020

Front. Cardiovasc. Med.

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The emergence of the COVID-19 virus and the subsequent pandemic have driven a great deal of research activity. The effects of COVID-19 are caused by the severe respiratory syndrome coronavirus 2 (SARS-CoV-2) and it is the underlying actions of SARs-CoV-2 virions on the endothelial glycocalyx that we consider here. One of the key factors in COVID-19 infection is its almost unique age-related profile, with a doubling in mortality every 10 years after the age of 50. The endothelial glycocalyx layer is essential in maintaining normal fluid homeostasis, but is fragile and prone to pathophysiological damage. It is physiologically significant in capillary microcirculation and in fluid distribution to the tissues. Human serum albumin (HSA), the most abundant protein in plasma, is created in the liver which also maintains its concentration, but this reduces by 10-15% after 50 years of age. HSA transports hormones, free fatty acids and maintains oncotic pressure, but SARS-CoV-2 virions bind competitively to HSA diminishing its normal transport function. Furthermore, hypoalbuminemia is frequently observed in patients with such conditions as diabetes, hypertension, and chronic heart failure, i.e., those most vulnerable to SARS-CoV-2 infection. Hypoalbuminemia, coagulopathy, and vascular disease have been linked in COVID-19 and have been shown to predict outcome independent of age and morbidity. Hypoalbuminemia is also known factor in sepsis and Acute respiratory distress syndrome (ARDS) occurs when fluids build-up in the alveoli and it is associated with sepsis, whose mechanism is systemic, being associated with the fluid and logistic mechanisms of the circulation. Glycocalyx damage is associated with changes plasma protein concentration, particularly HSA and blockage of albumin transport can produce the systemic symptoms seen in SARS-CoV-2 infection and sepsis. We therefore conclude that albumin binding to SARS-CoV-2 virions may inhibit the formation of the endothelial glycocalyx by inhibition of albumin transport binding sites. We postulate that albumin therapy to replace bound albumin might alleviate some of the symptoms leading to sepsis and that clinical trials to test this postulation should be initiated as a matter of urgency.

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“…The activity concentration in blood 1 h pi was as high as 32 ± 4% ID/g and decreased only 3.5-fold at 24 h pi. Such extension would not be possible for the relatively small ABD-RM26 conjugate (7 kDa) without interaction with albumin in blood circulation [ 35 , 36 , 37 ]. High activity concentration in blood contributed to elevated activity uptake in non-targeted organs (see Figure 8 ).…”

Section: Discussionmentioning

confidence: 99%

Preclinical Evaluation of the GRPR-Targeting Antagonist RM26 Conjugated to the Albumin-Binding Domain for GRPR-Targeting Therapy of Cancer

et al. 2020

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The targeting of gastrin-releasing peptide receptors (GRPR) was recently proposed for targeted therapy, e.g., radiotherapy. Multiple and frequent injections of peptide-based therapeutic agents would be required due to rapid blood clearance. By conjugation of the GRPR antagonist RM26 (D-Phe-Gln-Trp-Ala-Val-Gly-His-Sta-Leu-NH2) to an ABD (albumin-binding domain), we aimed to extend the blood circulation of peptides. The synthesized conjugate DOTA-ABD-RM26 was labelled with indium-111 and evaluated in vitro and in vivo. The labelled conjugate was stable in PBS and retained specificity and its antagonistic function against GRPR. The half-maximal inhibitory concentration (IC50) of natIn-DOTA-ABD-RM26 in the presence of human serum albumin was 49 ± 5 nM. [111In]In-DOTA-ABD-RM26 had a significantly longer residence time in blood and in tumors (without a significant decrease of up to 144 h pi) than the parental RM26 peptide. We conclude that the ABD-RM26 conjugate can be used for GRPR-targeted therapy and delivery of cytotoxic drugs. However, the undesirable elevated activity uptake in kidneys abolishes its use for radionuclide therapy. This proof-of-principle study justified further optimization of the molecular design of the ABD-RM26 conjugate.

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Albumin-Binding PSMA Ligands: Implications for Expanding the Therapeutic Window

Cited by 54 publications

References 24 publications

A Single Dose of ²²⁵Ac-RPS-074 Induces a Complete Tumor Response in an LNCaP Xenograft Model

A Single Dose of ²²⁵Ac-RPS-074 Induces a Complete Tumor Response in an LNCaP Xenograft Model

SARS-CoV-2 Bound Human Serum Albumin and Systemic Septic Shock

Preclinical Evaluation of the GRPR-Targeting Antagonist RM26 Conjugated to the Albumin-Binding Domain for GRPR-Targeting Therapy of Cancer

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Albumin-Binding PSMA Ligands: Implications for Expanding the Therapeutic Window

Cited by 54 publications

References 24 publications

A Single Dose of 225Ac-RPS-074 Induces a Complete Tumor Response in an LNCaP Xenograft Model

A Single Dose of 225Ac-RPS-074 Induces a Complete Tumor Response in an LNCaP Xenograft Model

SARS-CoV-2 Bound Human Serum Albumin and Systemic Septic Shock

Preclinical Evaluation of the GRPR-Targeting Antagonist RM26 Conjugated to the Albumin-Binding Domain for GRPR-Targeting Therapy of Cancer

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Product

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A Single Dose of ²²⁵Ac-RPS-074 Induces a Complete Tumor Response in an LNCaP Xenograft Model

A Single Dose of ²²⁵Ac-RPS-074 Induces a Complete Tumor Response in an LNCaP Xenograft Model