Molecular Design of HER3-Targeting Affibody Molecules: Influence of Chelator and Presence of HEHEHE-Tag on Biodistribution of 68Ga-Labeled Tracers

Leitao, Charles Dahlsson; Rinne, Sara S.; Mitran, Bogdan; Vorobyeva, Anzhelika; Andersson, Ken G.; Tolmachev, Vladimir; Ståhl, Stefan; Löfblom, John; Orlova, Anna

doi:10.3390/ijms20051080

Cited by 21 publications

(61 citation statements)

References 30 publications

(70 reference statements)

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“…The biodistribution of [ 68 Ga]-Ga-(HE) 3 -Z HER3 -NODAGA 3 h pi was directly compared with [ 57 Co]Co-(HE) 3 -Z HER3 -DOTA 24 h pi in the same batch of Balb/c nu/nu mice bearing BxPC-3 xenografts (Table S1, Figure 5). Data for [ 68 Ga]-Ga-(HE) 3 -Z HER3 -NODAGA was in agreement with previously published data [31]. Comparing [ 68 Ga]Ga-(HE) 3 -Z HER3 -NODAGA at 3 h pi with [ 57 Co]Co-(HE) 3 -Z HER3 -DOTA at 24 h pi, the cobalt-labeled variant had significantly lower activity concentration in blood, liver and stomach, and slightly higher uptake in tumor.…”

Section: In Vivo Evaluationsupporting

confidence: 91%

“…The different levels of uptake observed in the in vitro specificity test correlated to the different levels of HER3 expression, but no differences were observed in the cellular processing of the different conjugates. While low internalization rate seems to be characteristic for anti-HER3 affibody molecules, the observed rate is considerably lower than for the gallium-68 and indium-111-labeled analogs [26,31,43]. It could be speculated that cobalt-efflux mechanisms are triggered, which in addition to the already slow internalization of (HE) 3 -Z HER3 , partly affect the level of the internalized fraction [27].…”

Section: Discussionmentioning

confidence: 96%

“…It was hypothesized that an increased negative charge can reduce unspecific hepatic uptake and, therefore, enhance the tumorto-liver contrast [27]. This hypothesis was further supported by comparing the effect of differently charged radiometal-chelator complexes on the biodistribution of ZHER3 labeled with 68 Ga and 111 In and HER2-targeting affibody molecules [26,31,36].…”

Section: Radiolabeling and Stability Assessmentmentioning

confidence: 96%

“…The production and purification of the different affibody molecules (HE) 3 -Z HER3 -NOTA, (HE) 3 -Z HER3 -NODAGA, (HE) 3 -Z HER3 -DOTA, and (HE) 3 -Z HER3 -DOTAGA are described in Dahlsson Leitao et al [31]. An overview of the different chelators is depicted in Figure 1.…”

Section: Radiolabeling and Stability Assessmentmentioning

confidence: 99%

“…For PET imaging of HER3 expression, 18 F-and 68 Ga-labeled Z HER3 affibody molecules were able to visualize tumor uptake already 1 and 3 h pi in rodents. However, the tumor-to-liver contrast did not exceed 1 [21,31]. Unfortunately, these two commonly used PET isotopes have short half-lives (t 1/2 ( 18 F) = 110 min, t 1/2 ( 68 Ga) = 68 min) and are not suitable for next-day imaging.…”

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: In Vivo Evaluationsupporting

confidence: 91%

Section: Discussionmentioning

confidence: 96%

Section: Radiolabeling and Stability Assessmentmentioning

confidence: 96%

Section: Radiolabeling and Stability Assessmentmentioning

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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High‐throughput screening and biological display technology: Applications in molecular imaging

2023

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Molecular imaging plays important roles in many fields, including disease diagnosis, therapeutic efficacy evaluation, intraoperative imaging guidance, drug metabolism monitoring, and patient selection for appropriate treatment. As a key component, the targeting ligand determines the specificity, affinity, and in vivo performance of molecular imaging probes. In this review, high‐throughput screening and biological display platforms for the discovery of ligands applicable to molecular imaging are briefly reviewed. Basic information on ligand development for molecular imaging is first introduced, followed by a presentation of various selection platforms and typical or iterative cases. The features, advantages, limitations, and application scope of screening and display platforms are compared and discussed. Last, a basic selection strategy and a perspective for protein‐based ligands are provided.

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Osteosarcoma‐Derived Exosomes as Potential PET Imaging Nanocarriers for Lung Metastasis

Almeida

Fonseca

Ferreira

et al. 2022

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Lung metastases represent the most adverse clinical factor and rank as the leading cause of osteosarcoma‐related death. Nearly 80% of patients present lung micrometastasis at diagnosis not detected with current clinical tools. Herein, an exosome (EX)‐based imaging tool is developed for lung micrometastasis by positron emission tomography (PET) using osteosarcoma‐derived EXs as natural nanocarriers of the positron‐emitter copper‐64 (64Cu). Exosomes are isolated from metastatic osteosarcoma cells and functionalized with the macrocyclic chelator NODAGA for complexation with 64Cu. Surface functionalization has no effect on the physicochemical properties of EXs, or affinity for donor cells and endows them with favorable pharmacokinetics for in vivo studies. Whole‐body PET/magnetic resonance imaging (MRI) images in xenografted models show a specific accumulation of 64Cu‐NODAGA‐EXs in metastatic lesions as small as 2–3 mm or in a primary tumor, demonstrating the exquisite tropism of EXs for homotypic donor cells. The targetability for lung metastasis is also observed by optical imaging using indocyanine green (ICG)‐labeled EXs and D‐luciferin‐loaded EXs. These findings show that tumor‐derived EXs hold great potential as targeted imaging agents for the noninvasive detection of small lung metastasis by PET. This represents a step forward in the biomedical application of EXs in imaging diagnosis with increased translational potential.

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Molecular Design of HER3-Targeting Affibody Molecules: Influence of Chelator and Presence of HEHEHE-Tag on Biodistribution of 68Ga-Labeled Tracers

Cited by 21 publications

References 30 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

High‐throughput screening and biological display technology: Applications in molecular imaging

Osteosarcoma‐Derived Exosomes as Potential PET Imaging Nanocarriers for Lung Metastasis

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