HER3-Mediated Resistance to Hsp90 Inhibition Detected in Breast Cancer Xenografts by Affibody-Based PET Imaging

Martins, Carlos D.; Pieve, Chiara Da; Burley, Thomas A.; Smith, Rodney; Ciobota, Daniela M.; Allott, Louis; Harrington, Kevin; Oyen, Wim J.G.; Smith, Graham; Kramer‐Marek, Gabriela

doi:10.1158/1078-0432.ccr-17-2754

Cited by 22 publications

(24 citation statements)

References 53 publications

(60 reference statements)

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“…HER3 has evolved into an important molecular target in cancer. We and others have previously investigated the potential of radiolabeled affibody molecules as HER3-targeted imaging agents for PET and SPECT [15,16,[20][21][22]27]. It has been shown that an increase in the negative charge of the radionuclide-chelator complex can improve tumor-to-liver contrast for affibody molecules [26,36].…”

Section: Discussionmentioning

confidence: 99%

“…[ 89 Zr]Zr-DFO-Z HER3:8698 3 h pi reached a tumor-to-liver ratio of 1.18 ± 0.13. However, some release of the 89 Zr label was observed in vivo, resulting in a two-fold decrease in tumor uptake after 24 and, therefore, a decrease in tumor-to-liver contrast [22]. Compared with [ 111 In]In-Z HER3 -DOTAGA [26], tumor uptake of [ 57 Co]Co-(HE) 3 -Z HER3 -DOTA was slightly lower (3.4 ± 0.5 vs. 2.4 ± 0.4% ID/g at 24 h), but tumor-to-liver contrast of [ 57 Co]Co-(HE) 3 -Z HER3 -DOTA was higher at both time points, providing another argument for using cobalt-55 as a long-lived radiolabel for PET imaging.…”

Section: Discussionmentioning

confidence: 99%

“…Typically, a high contrast is obtained on the same day as the injection, as early as three to four hours post-injection (pi). We and others have previously shown the feasibility of anti-HER3 affibody molecules for imaging of HER3 expression with different radioisotopes for PET and SPECT [16,[20][21][22].…”

Section: Introductionmentioning

confidence: 99%

“…The long-lived PET isotope zirconium-89 (t 1/2 = 78.4 h) has been used for preclinical and clinical imaging of HER3 expression in combination with antibodies, and nanobodies [10,13,32]. Recently, a HER3-targeting affibody molecule was labeled with 89 Zr and used to detect changes in HER3 expression in response to treatment of breast cancer xenografts with an HSP90 inhibitor [22]. However, the fast kinetics of affibody molecules would also allow the use of PET isotopes with intermediate half-lives (shorter than 89 Zr but longer than 18 F and 68 Ga).…”

Section: Introductionmentioning

confidence: 99%

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Benefit of Later-Time-Point PET Imaging of HER3 Expression Using Optimized Radiocobalt-Labeled Affibody Molecules

Rinne

Leitao

Saleh-Nihad

et al. 2020

IJMS

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HER3-binding affibody molecules are a promising format for visualization of HER3 expression. Cobalt-55, a positron-emitting isotope, with a half-life of 17.5 h, allows for next-day imaging. We investigated the influence of the charge of the radiocobalt–chelator complex on the biodistribution of anti-HER3 affibody molecule (HE)3-ZHER3 and compared the best radiocobalt-labeled variant with a recently optimized gallium-labeled variant. Affibody conjugates (HE)3-ZHER3-X (X = NOTA, NODAGA, DOTA, DOTAGA) were labeled with [57Co]Co (surrogate for 55Co). Affinity measurements, binding specificity and cellular processing were studied in two HER3-expressing cancer cell lines. Biodistribution was studied 3 and 24 h post-injection (pi) in mice with HER3-expressing BxPC-3 xenografts and compared to [68Ga]Ga-(HE)3-ZHER3-NODAGA. Micro-single-photon emission tomography/computed tomography (microSPECT/CT) and micro-positron emission tomography/computed tomography (microPET/CT) imaging was performed 3 and 24 h pi. Stably labeled conjugates bound to HER3 with subnanomolar affinity. [57Co]Co-(HE)3-ZHER3-DOTA had the best tumor retention and a significantly lower concentration in blood than other conjugates, leading to superior tumor-to-blood and tumor-to-liver ratios 24 h pi. Compared to [68Ga]Ga-(HE)3-ZHER3-NODAGA 3 h pi, [57Co]Co-(HE)3-ZHER3-DOTA provided superior imaging contrast in liver 24 h pi. Concluding, the composition and charge of the [57Co]Co–chelator complex influenced the uptake in tumors and normal tissue. [57Co]Co-(HE)3-ZHER3-DOTA provided the best imaging properties among the cobalt-labeled conjugates. Delayed imaging of HER3 expression with [57Co]Co-(HE)3-ZHER3-DOTA improved imaging contrast compared to early-time-point imaging with [68Ga]Ga-(HE)3-ZHER3-NODAGA.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Benefit of Later-Time-Point PET Imaging of HER3 Expression Using Optimized Radiocobalt-Labeled Affibody Molecules

Rinne

Leitao

Saleh-Nihad

et al. 2020

IJMS

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“…Mice were administered the radioconjugate (12 µg in 100 µL of 0.9% sterile saline, 1.1-1.8 MBq/mouse) by intravenous tail vein injection and were anesthetized using an isoflurane/O 2 mixture (1.5%-2.0% v/v) approximately 5 min prior to imaging. Whole-body static PET images were acquired 1 h post-radioconjugate injection for the duration of 10 min, with a 358 to 664 keV energy window, followed by CT acquisition as previously described [26]. The image data were processed and reconstructed as previously reported [26].…”

Section: In Vivo Evaluationmentioning

confidence: 99%

Thiol-Reactive PODS-Bearing Bifunctional Chelators for the Development of EGFR-Targeting [18F]AlF-Affibody Conjugates

et al. 2020

Self Cite

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Site-selective bioconjugation of cysteine-containing peptides and proteins is currently achieved via a maleimide–thiol reaction (Michael addition). When maleimide-functionalized chelators are used and the resulting bioconjugates are subsequently radiolabeled, instability has been observed both during radiosynthesis and post-injection in vivo, reducing radiochemical yield and negatively impacting performance. Recently, a phenyloxadiazolyl methylsulfone derivative (PODS) was proposed as an alternative to maleimide for the site-selective conjugation and radiolabeling of proteins, demonstrating improved in vitro stability and in vivo performance. Therefore, we have synthesized two novel PODS-bearing bifunctional chelators (NOTA-PODS and NODAGA-PODS) and attached them to the EGFR-targeting affibody molecule ZEGFR:03115. After radiolabeling with the aluminum fluoride complex ([18F]AlF), both conjugates showed good stability in murine serum. When injected in high EGFR-expressing tumor-bearing mice, [18F]AlF-NOTA-PODS-ZEGFR:03115 and [18F]AlF-NODAGA-PODS-ZEGFR:03115 showed similar pharmacokinetics and a specific tumor uptake of 14.1 ± 5.3% and 16.7 ± 4.5% ID/g at 1 h post-injection, respectively. The current results are encouraging for using PODS as an alternative to maleimide-based thiol-selective bioconjugation reactions.

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Radiolabeled Affibody Molecules for PET Imaging

Da Pieve,

Kramer-Marek

2023

Methods in Molecular Biology

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HER3-Mediated Resistance to Hsp90 Inhibition Detected in Breast Cancer Xenografts by Affibody-Based PET Imaging

Cited by 22 publications

References 53 publications

Benefit of Later-Time-Point PET Imaging of HER3 Expression Using Optimized Radiocobalt-Labeled Affibody Molecules

Benefit of Later-Time-Point PET Imaging of HER3 Expression Using Optimized Radiocobalt-Labeled Affibody Molecules

Thiol-Reactive PODS-Bearing Bifunctional Chelators for the Development of EGFR-Targeting [18F]AlF-Affibody Conjugates

Radiolabeled Affibody Molecules for PET Imaging

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