Multiplex profiling of tumor‐associated proteolytic activity in serum of colorectal cancer patients

Yepes, Diego; Costina, Victor; Pilz, Lothar R.; Hofheinz, Ralf; Neumaier, Michael; Findeisen, Peter

doi:10.1002/prca.201300103

Cited by 8 publications

(5 citation statements)

References 26 publications

(38 reference statements)

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“…Monitoring protease activity as a biomarker of disease may be leveraged to overcome the lack of sensitivity and specificity of abundance-based blood biomarkers. 7 Common tools to measure protease activity often rely on cumbersome and infrastructure heavy analyses, such as fluorescence, [8][9][10] mass spectrometry, 11 or MRI. 12 Previously, we developed exogenously administered multiplexed protease-responsive nanoparticles that release small reporter probes into the urine in response to proteolytic cleavage in disease environments.…”

Section: Mainmentioning

confidence: 99%

Renal clearable catalytic gold nanoclusters for in vivo disease monitoring

et al. 2019

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Ultra-small gold nanoclusters (AuNCs) have emerged as agile probes for in vivo imaging, as they exhibit exceptional tumour accumulation and efficient renal clearance properties.However, their intrinsic catalytic activity, which can enable increased detection sensitivity, has yet to be explored for in vivo sensing. By exploiting the peroxidase-mimicking activity of AuNCs and the precise nanometer size filtration of the kidney, we designed multifunctional protease nanosensors that respond to disease microenvironments to produce a direct colorimetric urinary readout of disease state in less than 1 h. We monitored the catalytic activity of AuNCs in collected urine of a mouse model of colorectal cancer where tumour-bearing mice showed a 13-fold increase in colorimetric signal compared to healthy mice. Nanosensors were eliminated completely through hepatic and renal excretion within 4 weeks after injection with no evidence of toxicity. We envision that this modular approach will enable rapid detection of a diverse range of diseases by exploiting their specific enzymatic signatures.

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Section: Mainmentioning

confidence: 99%

Renal clearable catalytic gold nanoclusters for in vivo disease monitoring

et al. 2019

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“…Many routes to discover optimal substrates/spacers for FRET protease assays exist. These include a variety of combinatorial approaches (both solid 21,22 and solution based, 23 MS substrate profiling methods, 24,25 phage libraries 26 or substrate modification of known substrates, including direct screening on complex tumour tissues. 27 Many FRET peptide probes have been developed [28][29][30] and there are reviews covering this area so here we highlight some key and novel examples 14,19 with FRET based probes developed for legumain, 31 thrombin, 30 SARS-CoV protease, 32 Granzyme B 33 and Cathepsins, 34 among others.…”

Section: Optical Imagingmentioning

confidence: 99%

“…The tag-containing peptides co-eluted in chromatographic separations, while the combination of reporter peptides could be analysed by MS/MS. Findeisen developed a series of synthetic MS tagged reporter peptides 25,241,242 to help address a key challenge of protease profiling in complex biological samples, namely the risk of cleavage by non-specific peptidases, that are generally very abundant in complex samples. This was achieved by incorporating a flanking aminohexanoic acid groups in the peptide substrate that successfully reduced degradation by native exopeptidases.…”

Section: Ms Based Detectionmentioning

confidence: 99%

Peptide probes for proteases – innovations and applications for monitoring proteolytic activity

et al. 2022

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“…Finally, not only endogenous plasma proteins can be targeted for diagnostic use. Alternatively, the in vitro processing of synthetic peptides by disease‐related proteases can be monitored using MS‐based quantification .…”

Section: Applicationsmentioning

confidence: 99%

Clinical applications of MS‐based protein quantification

Sabbagh

Mindt

Neumaier

et al. 2016

Proteomics Clinical Apps

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Mass spectrometry-based assays are increasingly important in clinical laboratory medicine and nowadays are already commonly used in several areas of routine diagnostics. These include therapeutic drug monitoring, toxicology, endocrinology, pediatrics, and microbiology. Accordingly, some of the most common analyses are therapeutic drug monitoring of immunosuppressants, vitamin D, steroids, newborn screening, and bacterial identification. However, MS-based quantification of peptides and proteins for routine diagnostic use is rather rare up to now despite excellent analytical specificity and good sensitivity. Here, we want to give an overview over current fit-for-purpose assays for MS-based protein quantification. Advantages as well as challenges of this approach will be discussed with focus on feasibility for routine diagnostic use.

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Multiplex profiling of tumor‐associated proteolytic activity in serum of colorectal cancer patients

Abstract: Functional protease profiling with RPs might improve the laboratory-based diagnosis, monitoring and prognosis of malignant disease, and has to be evaluated thoroughly in future studies.

Cited by 8 publications

References 26 publications

Renal clearable catalytic gold nanoclusters for in vivo disease monitoring

Renal clearable catalytic gold nanoclusters for in vivo disease monitoring

Peptide probes for proteases – innovations and applications for monitoring proteolytic activity

Clinical applications of MS‐based protein quantification

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