Your search keyword '"Gómez-Caballero, Alberto"' showing total 2 results

1. Revealing novel biomarkers for diagnosing chronic kidney disease in pediatric patients.

Author

Benito, Sandra, Unceta, Nora, Maciejczyk, Mateusz, Sánchez-Ortega, Alicia, Taranta-Janusz, Katarzyna, Szulimowska, Julita, Zalewska, Anna, Andrade, Fernando, Gómez-Caballero, Alberto, Dubiela, Pawel, and Barrio, Ramón J.

Subjects

CHILD patients, CHRONIC kidney failure, RECEIVER operating characteristic curves, BIOMARKERS, QUADRUPOLE ion trap mass spectrometry, GLOMERULAR filtration rate

Abstract

Pediatric chronic kidney disease (CKD) is a clinical condition characterized by progressive renal function deterioration. CKD diagnosis is based on glomerular filtration rate, but its reliability is limited, especially at the early stages. New potential biomarkers (citrulline (CIT), symmetric dimethylarginine (SDMA), S-adenosylmethionine (SAM), n-butyrylcarnitine (nC4), cis-4-decenoylcarnitine, sphingosine-1-phosphate and bilirubin) in addition to creatinine (CNN) have been proposed for early diagnosis. To verify the clinical value of these biomarkers we performed a comprehensive targeted metabolomics study on a representative cohort of CKD and healthy pediatric patients. Sixty-seven children with CKD and forty-five healthy children have been enrolled in the study. Targeted metabolomics based on liquid chromatography-triple quadrupole mass spectrometry has been used for serum and plasma samples analysis. Univariate data analysis showed statistically significant differences (p < 0.05) in the concentration of CNN, CIT, SDMA, and nC4 among healthy and CKD pediatric patients. The predictive ability of the proposed biomarkers was also confirmed through specificity and sensitivity expressed in Receiver Operating Characteristic curves (AUC = 0.909). In the group of early CKD pediatric patients, AUC of 0.831 was obtained, improving the diagnostic reliability of CNN alone. Moreover, the models built on combined CIT, nC4, SDMA, and CNN allowed to distinguish CKD patients from healthy control regardless of blood matrix type (serum or plasma). Our data demonstrate potential biomarkers in the diagnosis of early CKD stages. [ABSTRACT FROM AUTHOR]

Published

2024

2. Solid-phase synthesis of imprinted nanoparticles as artificial antibodies against the C-terminus of the cannabinoid CB1 receptor: exploring a viable alternative for bioanalysis.

Author

Gómez-Caballero, Alberto, Elejaga-Jimeno, Ainhoa, García del Caño, Gontzal, Unceta, Nora, Guerreiro, Antonio, Saumell-Esnaola, Miquel, Sallés, Joan, Goicolea, M. Aránzazu, and Barrio, Ramón J.

Subjects

*SYNTHETIC antibodies, *SOLID-phase synthesis, *CHIMERIC proteins, *CANNABINOID receptors, *RECOMBINANT proteins, *CRITICAL temperature

Abstract

The production of artificial anti-CB1 antibodies in nanoparticle format is described using the solid-phase imprinting approach. Instead of whole protein imprinting, a linear C-terminus sequence of the receptor comprising 15 amino acids (458-KVTMSVSTDTSAEAL-472) has been used as template, in accordance with the epitope imprinting approach. This sequence is located intracellularly, and it is involved in coupling to Gi/o proteins, being responsible for CB1 receptor desensitisation and internalisation. Developed molecularly imprinted materials were found to be in the nanometre scale, with a particle size of 126.4 ± 10.5 nm at pH 3 (25 ºC) and spherical shape. It was also observed that the size was sensible to temperature changes being reduced to 106.3 ± 15.2 nm at 35 °C. Lower critical solution temperature of this polymer was found to be ≈ 33.4 °C. The affinity and selectivity of the artificial antibody were assessed through dot blot and Western blot experiments. For the latter, recombinant fusion proteins GST-CB1414-472 and GST-CB1414-442 were produced to work respectively as target and negative control proteins. The control protein did not carry the target epitope for being devoid of last 30 amino acids at the C-terminus. The results demonstrated that the anti-CB1 material recognised selectively the target protein, thanks to the presence of the 15-amino acid sequence selected as epitope, which revealed that binding occurred at the C-terminus of the receptor itself. The methodology presented may pave the way for the development of novel imprinted nanomaterials for other proteins included in the superfamily of the G-protein-coupled receptors (GPCR). [ABSTRACT FROM AUTHOR]

Published

2021