Real-time analysis of uptake and bioactivatable cleavage of luciferin-transporter conjugates in transgenic reporter mice

Wender, Paul A.; Goun, Elena A.; Jones, Lisa; Pillow, Thomas H.; Rothbard, Jonathan B.; Shinde, Rajesh; Contag, Christopher H.

doi:10.1073/pnas.0703919104

Cited by 80 publications

(69 citation statements)

References 45 publications

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“…Related strategies have been employed for assaying enzyme activity (33)(34)(35)(36)(37)(38) and cell-penetrating peptide transport efficiency (39), but these strategies have not been used for smallmolecule detection. Alkylation of firefly luciferin at the phenolic position prevents signal production even when luciferin's reactive carboxylic acid moiety remains unaltered (40).…”

Section: Resultsmentioning

confidence: 99%

In vivo imaging of hydrogen peroxide production in a murine tumor model with a chemoselective bioluminescent reporter

Bittner¹,

Dubikovskaya²,

Bertozzi

et al. 2010

Proc. Natl. Acad. Sci. U.S.A.

359

311

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Living organisms produce hydrogen peroxide (H 2 O 2 ) to kill invading pathogens and for cellular signaling, but aberrant generation of this reactive oxygen species is a hallmark of oxidative stress and inflammation in aging, injury, and disease. The effects of H 2 O 2 on the overall health of living animals remain elusive, in part owing to a dearth of methods for studying this transient small molecule in vivo. Here we report the design, synthesis, and in vivo applications of Peroxy Caged Luciferin-1 (PCL-1), a chemoselective bioluminescent probe for the real-time detection of H 2 O 2 within living animals. PCL-1 is a boronic acid-caged firefly luciferin molecule that selectively reacts with H 2 O 2 to release firefly luciferin, which triggers a bioluminescent response in the presence of firefly luciferase. The high sensitivity and selectivity of PCL-1 for H 2 O 2 , combined with the favorable properties of bioluminescence for in vivo imaging, afford a unique technology for real-time detection of basal levels of H 2 O 2 generated in healthy, living mice. Moreover, we demonstrate the efficacy of PCL-1 for monitoring physiological fluctuations in H 2 O 2 levels by directly imaging elevations in H 2 O 2 within testosterone-stimulated tumor xenografts in vivo. The ability to chemoselectively monitor H 2 O 2 fluxes in real time in living animals offers opportunities to dissect H 2 O 2 ’s disparate contributions to health, aging, and disease.

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Section: Resultsmentioning

confidence: 99%

In vivo imaging of hydrogen peroxide production in a murine tumor model with a chemoselective bioluminescent reporter

Bittner¹,

Dubikovskaya²,

Bertozzi

et al. 2010

Proc. Natl. Acad. Sci. U.S.A.

359

311

View full text Add to dashboard Cite

show abstract

“…Recently, we have also reported an imaging method that provides, for the first time, quantification of transporter-conjugate uptake and cargo release in real-time in both cells and animal models [103]. This method uses luciferase-transfected cells and transgenic (luciferase) reporter mice and whole-body imaging, allowing non-invasive quantification of transporter-conjugate uptake and probe (luciferin) release in real-time.…”

Section: Mechanisms Of Uptakementioning

confidence: 99%

The design of guanidinium-rich transporters and their internalization mechanisms

Wender

Galliher

Goun

et al. 2008

Advanced Drug Delivery Reviews

Self Cite

373

337

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The ability of a drug or probe to cross a biological barrier has historically been viewed to be a function of its intrinsic physical properties. This view has largely restricted drug design and selection to agents within a narrow log P range. Molecular transporters offer a strategy to circumvent these restrictions. In the case of guanidinium-rich transporters (GRTs), a typically highly water-soluble conjugate is found to readily pass through the non-polar membrane of a cell and for some across tissue barriers. This activity opens a field of opportunities for the use of GRTs to enable delivery of polar and nonpolar drugs or probes as well as to enhance uptake of those of intermediate polarity. The field of transporter enabled or enhanced uptake has grown dramatically in the last decade. Some GRT drug conjugates have been advanced into clinical trials. This review will provide an overview of recent work pertinent to the design and mechanism of uptake of GRTs.

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“…As a prelude to animal studies with Taxol conjugates, a third small-molecule system, luciferin, the substrate for firefly luciferase, was used as a drug surrogate to compare the biodistribution and pharmacokinetics of the r8 drug surrogate conjugate and the surrogate alone. Luciferin and luciferin conjugated to r8 (7) (38,39), at concentrations equimolar to those used in the studies with Taxol (5 mg/kg), were delivered via i.p. injection into transgenic mice ubiquitously expressing firefly luciferase (Fig.…”

Section: Biodistribution and Pharmacokinetics Of An Octaarginine-lucimentioning

confidence: 99%

Overcoming multidrug resistance of small-molecule therapeutics through conjugation with releasable octaarginine transporters

Dubikovskaya¹,

Thorne

Pillow³

et al. 2008

Proc. Natl. Acad. Sci. U.S.A.

Self Cite

219

213

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Many cancer therapeutic agents elicit resistance that renders them ineffective and often produces cross-resistance to other drugs. One of the most common mechanisms of resistance involves P-glycoprotein (Pgp)-mediated drug efflux. To address this problem, new agents have been sought that are less prone to inducing resistance and less likely to serve as substrates for Pgp efflux. An alternative to this approach is to deliver established agents as molecular transporter conjugates into cells through a mechanism that circumvents Pgp-mediated efflux and allows for release of free drug only after cell entry. Here we report that the widely used chemotherapeutic agent Taxol, ineffective against Taxol-resistant human ovarian cancer cell lines, can be incorporated into a releasable octaarginine conjugate that is effective against the same Taxolresistant cell lines. It is significant that the ability of the Taxol conjugates to overcome Taxol resistance is observed both in cell culture and in animal models of ovarian cancer. The generality and mechanistic basis for this effect were also explored with coelenterazine, a Pgp substrate. Although coelenterazine itself does not enter cells because of Pgp efflux, its octaarginine conjugate does so readily. This approach shows generality for overcoming the multidrug resistance elicited by small-molecule cancer chemotherapeutics and could improve the prognosis for many patients with cancer and fundamentally alter search strategies for novel therapeutic agents that are effective against resistant disease.ovarian cancer ͉ Pgp ͉ Taxol ͉ imaging ͉ luciferase

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Real-time analysis of uptake and bioactivatable cleavage of luciferin-transporter conjugates in transgenic reporter mice

Cited by 80 publications

References 45 publications

In vivo imaging of hydrogen peroxide production in a murine tumor model with a chemoselective bioluminescent reporter

In vivo imaging of hydrogen peroxide production in a murine tumor model with a chemoselective bioluminescent reporter

The design of guanidinium-rich transporters and their internalization mechanisms

Overcoming multidrug resistance of small-molecule therapeutics through conjugation with releasable octaarginine transporters

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