Preassembled Fluorescent Multivalent Probes for the Imaging of Anionic Membranes

Roland, Felicia M.; Peck, Evan M.; Rice, Douglas R.; Smith, Bradley D.

doi:10.1021/acs.bioconjchem.7b00012

Cited by 23 publications

(32 citation statements)

References 33 publications

(69 reference statements)

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“…The second major difference between POPC @CSP⊃6C and POPC @CSP⊃6Z liposomes was the fluorescence brightness. As shown in Figure B the fluorescence intensity of POPC @CSP⊃6Z liposomes was about four times lower, which matches previous observations that fluorescent ZnDPA complexes have a tendency to become self‐aggregated and self‐quenched on a membrane surface . As shown below, relief of this self‐quenching effect can be exploited to achieve target‐activated turn‐on fluorescence.…”

Section: Resultssupporting

confidence: 88%

“…As shown in Figure A the threading of 6C was complete within a few seconds, whereas the threading of 6Z required ≈20 minutes (Figure A). Previous studies have shown that the threading of 6Z by a dispersed, water‐soluble squaraine is fast so the slow formation of POPC @CSP⊃6Z must be a liposome surface effect. The most likely explanation is surface promoted association of the ZnDPA units in the newly docked 6Z with neighbouring CSP conjugates, driven by Lewis acid/base interactions between the Zn II cations and the electron‐rich squaraine oxygen atoms, as reported for related metal cation/dye association systems .…”

Section: Resultsmentioning

confidence: 99%

“…In short, a deep‐red fluorescent squaraine dye is encapsulated by a water‐soluble tetralactam macrocycle to give an extremely stable, threaded complex that is well suited for fluorescence imaging. To date, we have pre‐assembled fluorescent molecular probes that selectively target bone, dead/dying mammalian tissue, and various microbial species . One of the major advantages of Synthavidin self‐assembly is the capability of forming threaded complexes with long PEG chains appended to the ends of the squaraine dye .…”

Section: Introductionmentioning

confidence: 99%

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Non‐Covalent Assembly Method that Simultaneously Endows a Liposome Surface with Targeting Ligands, Protective PEG Chains, and Deep‐Red Fluorescence Reporter Groups

Shaw

Liu

Brennan

et al. 2017

Chemistry A European J

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A new self-assembly method is used to rapidly functionalize the surface of liposomes without perturbing the membrane integrity or causing leakage of the aqueous contents. The key molecule is a cholesterol-squaraine-PEG conjugate with three important structural elements: a cholesterol membrane anchor, a fluorescent squaraine docking station that allows rapid and high-affinity macrocycle threading, and a long PEG-2000 chain to provide steric shielding of the decorated liposome. The two-step method involves spontaneous insertion of the conjugate into the outer leaflet of pre-formed liposomes followed by squaraine threading with a tetralactam macrocycle that has appended targeting ligands. A macrocycle with six carboxylates permitted immobilization of intact fluorescent liposomes on the surface of cationic polymer beads, whereas a macrocycle with six zinc(II)-dipicolylamine units enabled selective targeting of anionic membranes, including agglutination of bacteria in the presence of human cells.

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Section: Resultssupporting

confidence: 88%

Section: Resultsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Non‐Covalent Assembly Method that Simultaneously Endows a Liposome Surface with Targeting Ligands, Protective PEG Chains, and Deep‐Red Fluorescence Reporter Groups

Shaw

Liu

Brennan

et al. 2017

Chemistry A European J

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“…Indeed, preliminary threading studies showedt hat near-quantitative threading occurred when H wasm ixed with one molar equivalent of R or C,o rH3H was mixed with two equivalents of R or C.I nF igure 1a,b are representative absorption spectra of the squaraine dyes before and after probe pre-assembly.T he absorption profile for free dimeric H3H is extremelyb road due to foldingo f the structure ands tacking of its two squaraine chromophores. [20,22] But after addition of macrocycle, near-quantitative threading and probe pre-assembly was indicated by the appearance of diagnostic narrow andr ed-shifted squaraine absorbance maxima. In Figure1c,d are two representative sets of absorption spectra showing the spectralc hanges that occur during the probe pre-assemblyp rocess.…”

Section: Resultsmentioning

confidence: 99%

“…Thisf inding is consistent with our previous work showingt hat Synthavidin pre-assembledp robesh ave sufficiently high kinetica nd thermodynamic stability to be effective biological imaging agents. [20][21][22] The cancert argeting capabilities of R'H and 2(R)'H3H were assessed using the integrin expressing cell lines OVCAR-4 and A549. OVCAR-4 is an excellent cell model of high-grade serous ovarian carcinoma because it has avery similar genomic sequence and response to chemotherapeutic drugs.…”

Section: Resultsmentioning

confidence: 99%

Non‐Covalently Pre‐Assembled High‐Performance Near‐Infrared Fluorescent Molecular Probes for Cancer Imaging

Shaw

Liu

Durán

et al. 2018

Chemistry A European J

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New fluorescent molecular probes, which can selectively target specific cell surface receptors, are needed for microscopy, in vivo imaging, and image guided surgery. The preparation of multivalent probes using standard synthetic chemistry can be a laborious process due to low reaction yields caused by steric effects. In this study, fluorescent molecular probes were prepared by a programmed non-covalent pre-assembly process that used a near-infrared fluorescent squaraine dye to thread a macrocycle bearing a cyclic arginine-glycine-aspartate peptide antagonist (cRGDfK) as a cancer targeting unit. Cell microscopy studies using OVCAR-4 (ovarian cancer) and A549 (lung cancer) cells that express high levels of the integrin αvβ3 or αvβ5 receptors, respectively, revealed a multivalent cell targeting effect. That is, there was comparatively more cell uptake of a pre-assembled probe equipped with two copies of the cRGDfK antagonist than a pre-assembled probe with only one appended cRGDfK antagonist. The remarkably high photostability and low phototoxicity of these near-infrared probes allowed for acquisition of long-term fluorescence movies showing endosome trafficking in living cells. In vivo near-infrared fluorescence imaging experiments compared the biodistribution of a targeted and untargeted probe in a xenograft mouse tumor model. The average tumor-to-muscle ratio for the pre-assembled targeted probe was 3.6 which matches the tumor targeting performance reported for analogous cRGDfK-based probes that were prepared entirely by covalent synthesis. The capability to excite these pre-assembled near-infrared fluorescent probes with blue or deep-red excitation light makes it possible to determine if a target site is located superficially or buried in tissue, a probe performance feature that is likely to be very helpful for eventual applications such as fluorescence guided surgery.

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Probes for Medical Imaging

Roland

Smith

2019

Supramolecular Chemistry in Water

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Preassembled Fluorescent Multivalent Probes for the Imaging of Anionic Membranes

Cited by 23 publications

References 33 publications

Non‐Covalent Assembly Method that Simultaneously Endows a Liposome Surface with Targeting Ligands, Protective PEG Chains, and Deep‐Red Fluorescence Reporter Groups

Non‐Covalent Assembly Method that Simultaneously Endows a Liposome Surface with Targeting Ligands, Protective PEG Chains, and Deep‐Red Fluorescence Reporter Groups

Non‐Covalently Pre‐Assembled High‐Performance Near‐Infrared Fluorescent Molecular Probes for Cancer Imaging

Probes for Medical Imaging

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