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      In vivo Iron-Based Coordination Assembly for Disease Diagnosis and Treatment

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            Abstract

            Advances in in vivo iron-based coordination assembly have enabled the simultaneous detection and treatment of iron-overload disorders. Specific interactions between local FeIII and organic ligands (e.g., indocyanine green and lecithin) facilitate magnetic resonance imaging with enhanced sensitivity and photoacoustic imaging with high contrast, thus overcoming the longstanding limitations of traditional iron quantification approaches. Moreover, enhanced iron depletion can also be achieved in murine genetic models of iron-overload disorders. These advances provide great promise in interdisciplinary leveraging of biology, medicine and materials science to design nanomedicines for addressing unmet clinical needs.

            Main article text

            Supramolecular assembly is ubiquitous in living systems, thus enabling construction of a range of fascinating structures with intricate biological functions that meet the essential needs of organisms [1, 2]. A typical example is metal-organic coordination assembly: in the light-harvesting complexes of photosynthetic systems, chromophores with metal-ion centers are assembled via coordination with histidineimidazole in proteins, thus forming particular arrangements that absorb light energy [3]. Furthermore, phenolic-iron coordination bonding has been implicated in various properties (e.g., mechanical and adhesive functions) of mussel byssus cuticle [4]. These natural phenomena may provide valuable inspiration for developing metal-organic-assembly materials and strategies for biomedical applications [57].

            Given the unique chemistry and biological functions of iron, recent research endeavors have paid particular attention to iron-based supramolecular assembly in vitro and in vivo, aiming at the development of desirable agents and nanomaterials for disease diagnosis and treatment [8, 9]. In in biological systems, iron ions are usually bound to molecules with electron-donating atoms (e.g., oxygen and sulfur). This characteristic has inspired pioneering work on in vitro nanomaterial assembly using iron-based coordination, wherein interactions between FeIII and various oxygen- and/or sulfur-containing therapeutics lead to the assembly of multifunctional theranostic nanoparticles. For example, co-assembly of photosensitizers (sinoporphyrin sodium) and chemotherapeutics (doxorubicin) with FeIII has enabled the formulation of metal-organic nanodrugs [10]. The reversible nature of coordination bonding has enabled biological barriers to nanoparticle delivery to be overcome. The metal-organic nanodrugs maintain their structures in the blood circulation under neutral pH (∼ 4) but steadily decompose into small drug complexes under the acidic (pH 5.5) tumor microenvironment, thereby enhancing intratumor drug permeability for effective image-guided photodynamic/chemo combinational therapy.

            To address the limited tissue penetration of photodynamic therapeutics, researchers have engineered metal-organic nanostructures for cancer sonodynamic therapy using ultrasound, whose deep tissue penetration triggers generation of reactive oxygen species (ROS), which kill cancer cells [11, 12]. Several smart cancer sonotheranostics have been fabricated through co-assembly of FeIII and organic sonosensitizers with a sulfonate group [e.g., meso-tetrakis (4-sulfonatophenyl) porphyrin, indocyanine green (ICG)], and other compounds and therapeutics [13, 14]. In a recent study, Lin et al. have reported microbubbles (MBs) loaded with FeIII/ICG coordination complexes for cancer sonotheranostics [14]. Ultrasound not only triggers in situ conversion of MBs into small FeIII/ICG nanocomplexes with better tissue penetration but also induces transient opening of leaky tumor vessels. These multiple benefits contribute to a 1.3-fold enhancement in tumoral deposition of FeIII/ICG@MBs, thus increasing ultrasound-mediated ROS generation for tumor ablation.

            Encouraged by the positive results regarding in vitro material assembly, Lin et al. subsequently applied in vivo iron-based assembly to noninvasive diagnosis and treatment of iron-overload diseases ( Figure 1 ) [15]. Iron-overloaded organs have abundant FeIII ions available for assembly with administered organic ligands and/or dyes. Such in situ assembly can alter iron and ligand forms (e.g., from free to aggregated), thus amplifying alterations in molecular-imaging signals and enabling iron detection. Specifically, the authors have designed an elegant ICG/lecithin (ICG/Leci) system in which the interaction between ICG and local FeIII in the iron-overloaded liver is accelerated by co-administered Leci, thus forming FeIII/ICG/Leci aggregates. The free-to-aggregate conversion by the ICG/Leci system offers several notable advantages as multimodal theranostics: ⅰ) the FeIII/ICG/Leci aggregation obstructs the water exchange rate with FeIII and significantly decreases MRI signals in the iron-overloaded liver, thereby enabling the detection of FeIII through MRI; ⅱ) π-π stacking between ICG and Leci results in UV-visible absorption at 890 nm, thus allowing for FeIII quantification through photoacoustic imaging with strong contrast and high sensitivity; ⅲ) the FeIII/ICG/Leci assembly alters the iron excretion pathway and facilitates twice the iron depletion of deferoxamine (a commonly investigated iron chelator), thus achieving better kinetics while avoiding toxicity.

            Figure 1

            Schematic graph showing recent advances in iron-based coordination assembly, from nanotherapeutic assembly in vitro to in situ iron-based assembly in vivo for iron quantification and depletion [15].

            This study provides a promising example of how iron-based coordination assembly can be leveraged to address unmet clinical needs. Liver biopsy, which remains the current gold standard for diagnosis of iron-overload diseases, is limited by sampling errors due to the nonuniform iron distribution in organs, and the possible risk of hospitalization (1–3%) [16]. Although MRI is becoming a more acceptable approach, its low sensitivity restricts its accuracy in iron quantification. The developed ICG/Leci system, with its enhanced MRI sensitivity and superior photoacoustic-imaging contrast, may aid in addressing the above issues and providing accurate, noninvasive diagnosis of iron-overloaded liver. When coupled with augmented iron depletion, the ICG/Leci system offers a powerful imaging-guided theranostic platform for iron-overload disorders. Interdisciplinary knowledge is highly desired for nanomedicine design, in which the properties of agents and nanomaterials are tailored according to biological and medical needs. This successful work is expected to inspire the development of more smart probes based on metal-organic assembly for diagnosis and therapeutic purposes.

            Conflicts of interest

            The authors declare that they have no conflicts of interest.

            References

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            2. , , , . Self-assembly in nature: using the principles of nature to create complex nanobiomaterials. Wiley Interdiscip Rev Nanomed Nanobiotechnol 2013;5:582–612. [PMID: 23929805 DOI: 10.1039/c7cs90102j]

            3. , , , , . Material science lesson from the biological photosystem. Nano Converg 2016;3:19. [PMID: 28191429 DOI: 10.1186/s40580-016-0079-5]

            4. , , , , , et al. Metal coordination-mediated functional grading and self-healing in mussel byssus cuticle. Adv Sci 2019;6:1902043. [PMID: 31832326 DOI: 10.1002/advs.201902043]

            5. , , , , , et al. Metal–organic framework-based stimuli-responsive systems for drug delivery. Adv Sci 2019;6:1801526. [PMID: 30643728 DOI: 10.1002/advs.201801526]

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            13. , , , , , et al. Fe(III)-porphyrin sonotheranostics: a green triple-regulated ROS generation nanoplatform for enhanced cancer imaging and therapy. Adv Funct Mater 2019;29:1904056. [DOI: 10.1002/adfm.201904056]

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            15. , , , , , et al. Repurposing ICG enables MR/PA imaging signal amplification and iron depletion for iron-overload disorders. Sci Adv 2021;7(51):eabl5862. [PMID: 34919434 DOI: 10.1126/sciadv.abl5862]

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            Author and article information

            Journal
            BIOI
            BIO Integration
            BIOI
            Compuscript (Ireland )
            2712-0082
            2712-0074
            August 2023
            01 July 2022
            : 4
            : 2
            : 70-72
            Affiliations
            [1] 1State Key Laboratory of Molecular Vaccinology and Molecular Diagnostics & Center for Molecular Imaging and Translational Medicine, School of Public Health, Xiamen University, Xiamen 361102, China
            [2] 2Faculty of Health Sciences, University of Macau, Taipa, Macau SAR 999078, China
            Author notes
            *Corresponding to: Gang Liu, E-mail: gangliu.cmitm@ 123456xmu.edu.cn
            Article
            bioi20220016
            10.15212/bioi-2022-0016
            d56ea42e-5f9b-414b-95b1-700c2d15707d
            Copyright © 2023 The Authors

            This is an open access article distributed under the terms of the Creative Commons Attribution License ( https://creativecommons.org/licenses/by/4.0/). See https://bio-integration.org/copyright-and-permissions/

            History
            : 01 May 2022
            : 01 June 2022
            : 16 June 2022
            Funding
            Funded by: Major State Basic Research Development Program of China
            Award ID: 2017YFA0205201
            Funded by: National Natural Science Foundation of China
            Award ID: 81925019
            Funded by: National Natural Science Foundation of China
            Award ID: U1705281
            Funded by: Fundamental Research Funds for the Central Universities
            Award ID: 20720190088
            Funded by: Fundamental Research Funds for the Central Universities
            Award ID: 20720200019
            Funded by: China Postdoctoral Science Foundation
            Award ID: 2020TQ0181
            Funded by: China Postdoctoral Science Foundation
            Award ID: 2021M690096
            Funded by: Program for New Century Excellent Talents in University, China
            Award ID: NCET-13-0502
            This work was supported by the Major State Basic Research Development Program of China (2017YFA0205201), the National Natural Science Foundation of China (81925019 and U1705281), the Fundamental Research Funds for the Central Universities (20720190088 and 20720200019), the China Postdoctoral Science Foundation (2020TQ0181 and 2021M690096) and the Program for New Century Excellent Talents in University, China (NCET-13-0502).
            Categories
            Perspective/Opinion

            Medicine,Molecular medicine,Radiology & Imaging,Biotechnology,Pharmacology & Pharmaceutical medicine,Microscopy & Imaging
            theranostics,multimodal molecular imaging,iron-based coordination assembly,In vivo assembly

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