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1. Evaluación de la supervivencia de los pacientes con cáncer de recto metastásico mediante parámetros radiómicos y volumétricos de la PET/TC con [18F]FDG de estadificación.

Author

Agüloğlu, N. and Aksu, A.

Abstract

El objetivo de este estudio es predecir el pronóstico de pacientes con cáncer de recto metastásico (CRM) mediante la obtención de un modelo con algoritmos de aprendizaje automático (AA) a través de datos volumétricos y radiómicos obtenidos de la PET/TC basal. Pacientes con CRM que se sometieron a imágenes PET/TC con [18F]FDG para estadificación en nuestro hospital entre enero 2015 y enero de 2021 se evaluaron mediante el software LIFEx. El volumen de interés (VOI) del tumor primario fue generado. Además, se evaluaron los valores del volumen metabólico tumoral total (tMTV) y la glucólisis de lesión total (TLG) de los focos tumorales en todo el cuerpo. Se evaluaron los datos clínicos y radiómicos con algoritmos de AA para crear un modelo que predijera la supervivencia. Se investigaron asociaciones significativas entre estas características y la supervivencia a 1 y 2 años. El algoritmo de bosque aleatorizado fue el algoritmo más exitoso para predecir la supervivencia a 2 años (AUC: 0,843; PRC: 0,822 y CCM: 0,583). Los valores de tMTV y tTLG tuvieron éxito en la predicción de la supervivencia a un año (p 0,002 y 0,007, respectivamente). Además del importante papel de la PET/TC con [18F]FDG en la estadificación de pacientes con CRM, este estudio muestra que es posible predecir la supervivencia con métodos de AA, con parámetros obtenidos mediante el análisis de textura a partir del tumor primario y parámetros volumétricos de todo el cuerpo. The aim of this study was to predict the prognosis in patients with metastatic rectal cancer (mRC) by obtaining a model with machine learning (ML) algorithms through volumetric and radiomic data obtained from baseline 18-Fluorine Fluorodeoxyglucose ([18F]FDG) positron emission tomography/computed tomography (PET/CT) images. Sixty-two patients with mRC who underwent [18F]FDG PET/CT imaging for staging between January 2015 and January 2021 were evaluated using LIFEx software. The volume of interest (VOI) of the primary tumor was generated and volumetric and textural features were obtained from this VOI. In addition, the total metabolic tumor volume (tMTV) and total lesion glycolysis (TLG) values of tumor foci in the whole body were evaluated. Clinical and radiomic data were evaluated with ML algorithms to create a model that predicts survival. Significant associations between these features and 1- and 2-year survival were investigated. The random forest algorithm was the most successful in predicting 2-year survival (AUC: 0.843, precision-recall curve: 0.822 and Matthew's correlation coefficient: 0.583). The model obtained with this algorithm was able to predict 49 patients with 79.03% accuracy. While tMTV and TLG values were successful in predicting 1-year survival (p: 0.002 and 0.007, respectively), texture characteristics of the primary tumor did not show a significant relationship with 1-year survival. In addition to the important role of [18F]FDG PET/CT in staging patients with mRC, this study shows that it is possible to predict survival with ML methods, with parameters obtained using texture analysis of the primary tumor and whole body volumetric parameters. [ABSTRACT FROM AUTHOR]

Published
2023
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2. Evaluation of survival of the patients with metastatic rectal cancer by staging 18 F-FDG PET/CT radiomic and volumetric parameters.

Author

Agüloğlu N and Aksu A

Subjects
Humans, Fluorodeoxyglucose F18, Prognosis, Positron Emission Tomography Computed Tomography methods, Rectal Neoplasms
Abstract

Objective: The aim of this study is to predict the prognosis in patients with metastatic rectal cancer (mRC) by obtaining a model with machine learning (ML) algorithms through volumetric and radiomic data obtained from baseline 18-Fluorine Fluorodeoxyglucose (18F-FDG) positron emission tomography/computed tomography (PET/CT) images., Methods: Sixty-two patients with mRC who underwent 18F-FDG PET/CT imaging for staging between January 2015 and January 2021 were evaluated using LIFEx software. The volume of interest (VOI) of the primary tumor was generated and volumetric and textural features were obtained from this VOI. In addition, metabolic tumor volume (tMTV) and total lesion glycolysis (tTLG) values of tumor foci in the whole body. Clinical and radiomic data were evaluated with ML algorithms to create a model that predicts survival. Significant associations between these features and 1-year and 2-year survival were investigated., Results: Random forest algorithm was the most successful algorithm in predicting 2-year survival (AUC: 0.843, PRC: 0.822, and MCC: 0.583). The model obtained with this algorithm was able to predict 49 patients with 79.03% accuracy. While tMTV and tTLG values were successful in predicting 1-year survival (p: 0.002 and 0.007, respectively), texture characteristics from the primary tumor did not show a significant relationship with 1-year survival., Conclusions: In addition to the important role of 18F-FDG PET/CT in staging patients with mRC, this study shows that it is possible to predict survival with ML methods, with parameters obtained using texture analysis from the primary tumor and whole body volumetric parameters., (Copyright © 2022 Sociedad Española de Medicina Nuclear e Imagen Molecular. Published by Elsevier España, S.L.U. All rights reserved.)

Published
2023
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3. Identificación de nuevos biomarcadores para cáncer colorrectal metastásico: análisis genómico y metabólomico

Author

González Flores, Encarnación, Prados Salazar, José Carlos, Melguizo Alonso, Consolación, and Universidad de Granada. Programa de Doctorado en Biomedicina

Subjects
Biomarcadores, Metastatic colorectal cancer, Cáncer colorrectal metastásico, Biomarkers
Abstract

El cáncer colorrectal (CCR) debe ser considerado como un auténtico problema de salud pública tanto por su incidencia, es el tercer tumor más frecuente en el mundo representando el 10 % del total de las neoplasias, como por su mortalidad que lo sitúa como la segunda causa de muerte por cáncer. En España y considerando ambos sexos, el CCR es el más tumor más frecuente superando en la actualidad al de mama y pulmón. A pesar de los importantes avances en el tratamiento del CCR en los últimos años y de la mejora en su diagnóstico precoz, un número muy importante de pacientes, entre un 20-25%, presentan enfermedad metastásica en el momento del diagnóstico y hasta un 50% desarrollan metástasis a lo largo de la evolución de la enfermedad. Por tanto, el diagnóstico precoz, así como el desarrollo de estrategias para determinar su pronóstico y la eficacia de la terapia aplicada, es un campo prioritario en la investigación oncológica. En este contexto, el conocimiento cada vez más profundo de la etiopatogenia del CCR, el carácter heterogéneo del mismo, y la demostración de que múltiples alteraciones tanto genéticas como epigenéticas son capaces de alterar los mecanismos de control de los procesos de proliferación , diferenciación y apoptosis celular, están dando paso, no sólo al uso de nuevas dianas moleculares que permitan un tratamiento más preciso y específico, sino a la determinación de nuevas biomoléculas, que usadas como biomarcadores, puedan indicarnos la presencia, la evolución y/o la respuesta al tratamiento de la enfermedad. Los biomarcadores tumorales, entendidos como entidades biológicas que puede ser detectadas en los diferentes medios orgánicos de pacientes con cáncer, son las moléculas que están permitiendo el seguimiento de la enfermedad monitorizando sus niveles, su diagnóstico (incluyendo métodos de screening poblacional), su pronóstico e incluso, el seguimiento de la respuesta terapéutica. En la actualidad, existe un déficit de marcadores precisos y sensibles para el cáncer en general y para el CCR en particular. Así, son muchos los estudios que han investigado como biomarcador en CCR, moléculas de DNA liberadas a sangre en procesos de apoptosis celular o paso de células vivas al torrente circulatorio (CTSs). Los exosomas, pequeñas vesículas envueltas por una bicapa lípidica que están implicados en la transferencia de miRNAs, ARMm y proteínas a una célula diana, también han sido propuestos como biomarcadores de esta enfermedad. Incluso la presencia en el suero de pacientes con CCR de determinadas proteínas ha sido analizada ampliamente, a pesar de lo cual, sólo CEA y CA-19-9 siguen siendo clínicamente utilizadas, aunque adolecen de una baja sensibilidad y especificidad. Múltiples estudios han sido también realizados para determinar miRNA en pacientes con CCR que sean específicos para su diagnóstico o pronóstico, pero sin resultados definitivos. Entre las moléculas más ampliamente analizadas como biomarcadores de CCR se encuentran la presencia de ARNm en sangre periférica. En este contexto, el ARNm de moléculas relacionas con el proceso de la angiogénesis han cobrado un gran interés en el CCR, habiéndose testado la sobreexpresión de moléculas como PTGS2 y GUCY2C como marcadores de la enfermedad o de la presencia de metástasis ocultas en pacientes con CCR. Por otra parte, la metabolómica, una disciplina que evalúa los metabolitos endógenos producidos por el organismo, esta revolucionado el campo de los biomarcadores para distintos tipos de patologías. Aplicada al cáncer, la metabolómica ofrece una representación molecular del fenotipo tumoral que puede servir para el diagnóstico, el pronóstico y la identificación de subgrupos relevantes desde un punto de vista clínico. Las células tumorales adaptan su metabolismo a una proliferación descontrolada que provoca alteraciones metabólicas que tiene su reflejo en la aparición o la modulación de los niveles de metabolitos. En el CCR, algunos metabolitos concretos (ácido betahidroxibutirato, cistamina, ácido aspártico, entre otros) han sido propuestos para el diagnóstico de CCR tanto en sangre como en orina, aunque la complejidad para detectarlos y su elevado coste hace necesarios más esfuerzos de investigación para llevarlos a la práctica clínica. En este contexto, nuestro trabajo ha tenido dos objetivos fundamentales: i) Por una parte, realizar un estudio de la utilidad de genes intensamente relacionados con el proceso de angiogénesis, fenómeno esencial en el crecimiento y la expansión metastásica de un tumor, como nuevos biomarcadores de fácil detección en sangre períferica o en suero de los pacientes con CCRm. Para ello hemos seleccionado cinco genes, GUCY2C, JAG1, PTGS2, PGF y MMP7, con demostrada relevancia en la angiogénesis y hemos determinado los niveles de ARN circulante tanto en suero como en células mononucleares de sangre periférica en un grupo de 59 pacientes con CCRm enfrentados a un grupo de 47 controles sanos. La presencia de estos marcadores en los fluidos biológicos fue realizada por una tecnología altamente sensible como es la dPCR que permitiría un fácil desarrollo de su aplicación clínica en un corto plazo de tiempo, mientras que el análisis del AUC se utilizó para estimar el valor predictivo de los biomarcadores tanto de forma individual como en combinaciones (firma biológica). ii) Por otra parte, hemos realizado un estudio para identificar biomarcadores basados en la determinación de metabolitos en suero de pacientes de CCRm que sea útil en el diagnóstico, pronóstico y seguimiento de estos pacientes. En este caso y basándonos en técnicas de metabolómica no dirigida, se han analizado los sueros de un grupo 65 pacientes con CCRm enfrentados a 60 controles sanos. Las muestras fueron sometidas a estudios mediante cromatografía líquida de fase inversa acoplada a espectrometría de masas de alta resolución (LC-HRMS), que nos permitió obtener una matriz para comparar controles sanos con pacientes con CCR. Los metabolitos obtenidos fuero analizados de forma individual y también en forma de “clúster” con el objeto de obtener una posible huella biológica., Colorectal cancer (CRC) must be considered a real public health problem both because of its incidence, it is the third most frequent tumour in the world, representing 10% of all neoplasms, and because of its mortality, which places it as the second leading cause of death from cancer. In Spain and considering both sexes, CRC is the most frequent tumour, currently surpassing breast and lung tumours. Despite the important advances in the treatment of CRC in recent years and the improvement in its early diagnosis, a very important number of patients, between 20- 25%, present metastatic disease at the time of diagnosis and up to 50 % develop metastases throughout the course of the disease. Therefore, the determination of the metastatic stage of the disease at an early stage, as well as the development of strategies to determine its prognosis and the effectiveness of the applied therapy, is a priority field in cancer research. In this context, the increasingly in-depth knowledge of the etiopathogenesis of CRC, its heterogeneous nature, and the demonstration that multiple genetic and epigenetic alterations are capable of altering the control mechanisms of proliferation, differentiation and apoptosis cellular, are giving way, not only to the use of new molecular targets that allow a more precise and specific treatment, but to the determination of new biomolecules, which, used as biomarkers, can indicate the presence, evolution and / or response to treatment of the illness. Tumour biomarkers, understood as biological entities that can be detected in the different organic environments of cancer patients, are the molecules that are allowing the follow-up of the disease by monitoring its levels, its diagnosis (including population screening methods), its prognosis and even the follow-up of the therapeutic response. At present, there is a shortage of precise and sensitive markers for cancer in general and for CRC in particular. Thus, there are many studies that have investigated as a biomarker in CRC, DNA molecules released into the blood in process of cellular apoptosis or passage of living cells into the circulatory stream (circulating tumor cells or CTSs). Exosomes, small vesicles surrounded by a lipid bilayer that are involved in the transfer of miRNAs, mRNAs and proteins to a target cell, have also been proposed as biomarkers of this disease. Even the presence in the serum of patients with CRC of certain proteins has been extensively analyzed, despite which, only CEA and CA-19-9 are still used clinically, although they suffer from low sensitivity and specificity. Multiple studies have also been carried out to determine microRNA in patients with CRC that are specific for their diagnosis or prognosis but without definitive results. Among the molecules most widely analysed as CRC biomarkers are the presence of messenger RNA (mRNA) in peripheral blood. In this context, the mRNA of molecules related to the angiogenesis process have gained great interest in CRC, having tested the overexpression of molecules such as PTGS2 and GUCY2C as markers of the disease or of the presence of hidden metastases in patients with CRC. On the other hand, metabolomics, a discipline that evaluates the endogenous metabolites produced by the body, has revolutionised the field of biomarkers for different types of pathologies. Applied to cancer, metabolomics offers a molecular representation of the tumour phenotype that can be used for diagnosis, prognosis, and identification of clinically relevant subgroups. Tumour cells adapt their metabolism to uncontrolled proliferation that causes metabolic alterations that are reflected in the appearance or modulation of metabolite levels. In CRC, some specific metabolites (beta-hydroxybutyrate acid, cystamine, aspartic acid, among others) have been proposed for the diagnosis of CRC in both blood and urine, although the complexity to detect them and their high cost require more research efforts to take them into clinical practice. In this context, our work has had two fundamental objectives: i) On the one hand, to carry out a study that the utility of genes intensely related by the angiogenesis process, an essential phenomenon in the growth and metastatic expansion of a tumor, as new biomarkers easily detected in peripheral blood or serum of patients with metastatic CRC. For this we have selected five genes, GUCY2C, JAG1, PTGS2, PGF and MMP7, with demonstrated relevance in angiogenesis and we have determined the levels of circulating RNA both in serum and in peripheral blood mononuclear cells in a group of 59 patients with metastatic RCC faced with a group of 47 healthy controls. The presence of these markers in biological fluids was carried out by a highly sensitive technology such as digital PCR (dPCR) that would allow an easy development of its clinical application in a short period of time, whilst the analysis of the area under the curve (AUC) was used to estimate the predictive value of biomarkers both individually and in combinations (biological signature). ii) On the other hand, we have carried out a study to identify biomarkers based on the determination of metabolites in the serum of metastatic CRC patients that is useful in the diagnosis, prognosis and follow-up of these patients. In this case, and based on undirected metabolomics techniques, the sera of a group of 65 patients with metastatic CRC compared to 60 healthy controls were analysed. The samples were subjected to studies by reverse phase liquid chromatography coupled to high resolution mass spectrometry (LC-HRMS), which allowed us to obtain a matrix to compare healthy controls with patients with CRC. The metabolites obtained were analyzed individually and also in the form of a "cluster" in order to obtain a possible biological trace., Tesis Univ. Granada.

Published
2021

4. First-line panitumumab plus FOLFOX4 or FOLFIRI in colorectal cancer with multiple or unresectable liver metastases: A randomised, phase II trial (PLANET-TTD)

Author

Carrato, Alfredo, Abad, Albert, Massuti, Bartomeu, Grávalos, Cristina, Escudero, Pilar, Longo Muñoz, Federico, Manzano, José Luis, Gómez, Auxiliadora, Safont, María José, Gallego, Javier, García-Paredes, Beatriz, Pericay, Carles, Dueñas, Rosario, Rivera, Fernando, Losa, Ferrán, Valladares Ayerbes, Manuel, González, Encarnación, Aranda, Enrique, Spanish Cooperative Group for the Treatment of Digestive Tumours (TTD), and Universitat Autònoma de Barcelona

Subjects
Male, 0301 basic medicine, Oncology, Cancer Research, fluorouracilo, Organoplatinum Compounds, astenia, Cáncer colorrectal metastásico, Leucovorin, Appetite, oncología médica, Medical Oncology, Gastroenterology, 0302 clinical medicine, FOLFOX, Antineoplastic Combined Chemotherapy Protocols, Skin, Aged, 80 and over, Metastatic colorectal cancer, Panitumumab, Liver Neoplasms, Hazard ratio, Antibodies, Monoclonal, First-line, Middle Aged, apetito, 030220 oncology & carcinogenesis, FOLFIRI, Female, Fluorouracil, Liver-limited disease, Colorectal Neoplasms, medicine.drug, Adult, medicine.medical_specialty, Neutropenia, neoplasias colorrectales, leucovorina, prurito, 03 medical and health sciences, Folinic acid, Internal medicine, medicine, Humans, Aged, business.industry, Pruritus, Resection, medicine.disease, Survival Analysis, piel, Oxaliplatin, Irinotecan, 030104 developmental biology, Spain, Asthenia, Camptothecin, business
Abstract

Background In first-line wild-type (WT)-Kirsten rat sarcoma viral oncogene homologue (KRAS) metastatic colorectal cancer (mCRC), panitumumab (Pmab) improves outcomes when added to FOLFOX [folinic acid, 5-fluorouracil, and oxaliplatin] or FOLFIRI [folinic acid, 5-fluorouracil, and irinotecan]. However no trial has directly compared these combinations. Methods Multicentre, open-label study in untreated patients ≥ 18 years with (WT)-KRAS mCRC and multiple or unresectable liver-limited disease (LLD) randomised to either Pmab-FOLFOX4 or Pmab-FOLFIRI. The primary end-point was objective response rate (ORR). Secondary end-points included liver metastases resection rate (R0 + R1), progression-free survival (PFS), overall survival (OS), adverse events and perioperative safety. Exploratory end-points were: response by RAS status, early tumour shrinkage (ETS) and depth of response (DpR) in WT-RAS patients. Results Data on 77 patients were analysed (38 Pmab-FOLFOX4; 39 Pmab-FOLFIRI; WT-RAS: 27/26, respectively). ORR was 74% with Pmab-FOLFOX4 and 67% with Pmab-FOLFIRI (WT-RAS: 78%/73%). Out of the above, 45% and 59% underwent surgical resection, respectively (WT-RAS: 37%/69%). The R0-R1 resection rate was 34%/46% (WT-RAS:26%/54%). Median PFS was 13/14 months (hazard ratio [HR] Pmab-FOLFIRI versus Pmab-FOLFOX4: 0.9; 95% confidence interval: [0.6–1.5]; WT-RAS:13/15; HR: 0.7 [0.4–1.3]). Median OS was 37/41 months (HR:1.0 [0.6–1.8]; WT-RAS: 39/49; HR:0.9 [0.4–1.9]). In WT-RAS patients with confirmed response, median DpR was 71%/66%, and 65%/77% of patients showed ETS ≥ 30%/ ≥ 20% at week 8, without significant differences between arms; these patients had longer median PFS and OS and higher resectability rates. Surgery was associated with longer survival. Perioperative and overall safety were similar, except for higher grade 3/4 neutropenia (40%/10%; p = 0.003) and neuropathy (13%/0%; p = 0.025) in the Pmab-FOLFOX4 arm. Conclusions In patients with WT-KRAS mCRC and LLD, both first-line Pmab-FOLFOX4 and Pmab-FOLFIRI resulted in high ORR and ETS, allowing potentially curative resection. No significant differences in efficacy were observed between the two regimens. (clinicaltrials.gov: NCT00885885 ).

Published
2017
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5. Análisis de costo-efectividad de panitumumab + FOLFOX en CCRm RAS-WT

Author

Juan Jesús Vargas Valencia and Mónica Elena Alva Esqueda

Subjects
Cancer Research, business.industry, Metastatic colorectal cancer, Panitumumab, Cáncer colorrectal metastásico, Bevacizumab, Oncology, Wild-type RAS, Medicine, RAS natural, business, Humanities, medicine.drug
Abstract

ResumenObjetivoEfectuar una evaluación de costo-efectividad del esquema panitumumab + FOLFOX como primera línea en pacientes con CCRm RAS-WT vs. el uso de bevacizumab + FOLFOX.MétodoMediante un modelo de Markov, se evaluó una cohorte hipotética de pacientes a través de 7 estados de salud en ciclos de transición de 2 semanas. La supervivencia libre de progresión (SLP) y la supervivencia global (SG) se tomaron del estudio PEAK. El uso de recursos se obtuvo de un panel de 5 oncólogos pertenecientes a 4 hospitales públicos. El costo incluye quimioterapia, seguimiento, eventos adversos, resección de metástasis, segunda línea, cuidados paliativos y gastos funerarios. Se aplican costos del IMSS, con una tasa de descuento del 5% a beneficios y costos con un horizonte a 5 años. Se realizó un análisis de minimización de costos vs. cetuximab debido a la equivalencia en SG según el estudio ASPECCT y resultados similares en SLP y SG en primera línea en población RAS-WT.ResultadosEl costo total con panitumumab es de $ 1,048,009.42 y de $ 872,201.70 con bevacizumab, con una media de 3.47 y 2.80 años de vida y una razón costo-efectividad promedio de $ 25,173 y $ 25,932, respectivamente, por mes de SG. De la proyección a 10 meses con la terapia anti-EGFR, el costo es de $ 779,873.60 y $ 1,119,871.90 con panitumumab y cetuximab, respectivamente, lo cual representa un ahorro de $ 339,998.30 (30.4%) por paciente.ConclusionesPanitumumab como primer tratamiento mejora los parámetros clínicos en pacientes con CCRm RAS-WT y presenta una razón costo-efectividad media similar a bevacizumab en dicha población. Con respecto a cetuximab, panitumumab constituye una estrategia costo-ahorradora para las instituciones de salud pública en México.AbstractObjectiveTo conduct a cost-effectiveness analysis of panitumumab+FOLFOX vs. bevacizumab+FOLFOX as first-line therapy in RAS-WT mCRC patients.MethodUsing a Markov model, a hypothetical cohort of patients was assessed throughout seven health stages in two-week transition cycles. Progression-free survival (PFS) and overall survival (OS) were taken from the PEAK trial. The use of resources was obtained from a panel of five oncologists at four public hospitals. The costs include chemotherapy, follow-up, adverse events, metastases resection, second-line therapy, palliative care, and funeral expenses. IMSS’ costs were applied, with costs and benefits discounted at 5% for a 5-year time line. A cost-minimisation analysis vs. cetuximab was performed due to the OS equivalence according to the ASPECCT trial and similar PFS and OS results as first-line in RAS-WT populations.ResultsTotal costs are $1,048,009.42 for panitumumab and $872,201.70 for bevacizumab with a mean of 3.47 and 2.80 years of life, and a mean cost-effectiveness ratio per month of OS of $25,173 and $25,932, respectively. The 10-month projection for anti-EGFR therapies reveals a total cost of $779,873.60 for panitumumab and $1,119,871.90 for cetuximab, which represents savings of $339,998.30 (30.4%) per patient.ConclusionsPanitumumab as first-line treatment improves clinical parameters in RAS-WT mCRC patients and has a mean cost-effectiveness ratio similar to bevacizumab in this population. Compared to cetuximab, panitumumab represents a cost-saving strategy for public healthcare institutions in Mexico.

Published
2015
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6. Predicting Outcome and Therapy Response in mCRC Patients Using an Indirect Method for CTCs Detection by a Multigene Expression Panel: A Multicentric Prospective Validation Study

Author

Vidal Insua, Yolanda, De La Cámara Gómez, Juan Cruz, Brozos Vázquez, Elena María, Fernández Montes, Ana, Vázquez Rivera, Francisca, Villanueva Silva, María José, Barbazán García, Jorge, Muinelo Romay , Laura, Candamio Folgar, Sonia, Abalo Piñeiro, Alicia, López López, Rafael, Abal Posada, Miguel, and Alonso Alconada, Lorena

Subjects
Células tumorales circulantes, neoplasias colorrectales, células neoplásicas circulantes, Cáncer colorrectal metastásico, Tumor maligno del colon, parte no especificada, Neoplastic Cells, Circulating, Disease-Free Survival, Detección temprana del cáncer, Survival Rate, detección precoz del cáncer, Biomarcadores, supervivencia sin enfermedad, tasa de supervivencia, Neoplasm Metastasis, Colorectal Neoplasms, Early Detection of Cancer, metástasis neoplásica, Biomarkers, Respuesta al tratamiento
Abstract

Colorectal cancer (CRC) is one of the major causes of cancer-related deaths. Early detection of tumor relapse is crucial for determining the most appropriate therapeutic management. In clinical practice, computed tomography (CT) is routinely used, but small tumor changes are difficult to visualize, and reliable blood-based prognostic and monitoring biomarkers are urgently needed. The aim of this study was to prospectively validate a gene expression panel (composed of GAPDH, VIL1, CLU, TIMP1, TLN1, LOXL3 and ZEB2) for detecting circulating tumor cells (CTCs) as prognostic and predictive tool in blood samples from 94 metastatic CRC (mCRC) patients. Patients with higher gene panel expression before treatment had a reduced progression-free survival (PFS) and overall-survival (OS) rates compared with patients with low expression (p = 0.003 and p ≤ 0.001, respectively). Patients with increased expression of CTCs markers during treatment presented PFS and OS times of 8.95 and 11.74 months, respectively, compared with 14.41 and 24.7 for patients presenting decreased expression (PFS; p = 0.020; OS; p ≤ 0.001). Patients classified as non-responders by CTCs with treatment, but classified as responders by CT scan, showed significantly shorter survival times (PFS: 8.53 vs. 11.70; OS: 10.37 vs. 24.13; months). In conclusion, our CTCs detection panel demonstrated efficacy for early treatment response assessment in mCRC patients, and with increased reliability compared to CT scan. ACIS (Axencia de Coñecemento en Saude); SERGAS. Cofinanced ERDF Funds 2007–2013

Published
2017

9. Eficacia de terapias biológicas de tipo anti-angiogénico en el cáncer colorrectal metastásico revisión sistemática de la literatura

Author

Salas, Carolina, Montañez Rivera, Edwin Alexander, Prieto Ruiz, Natalia, Salas, Carolina, Montañez Rivera, Edwin Alexander, and Prieto Ruiz, Natalia

Abstract

Introducción: El cáncer colorrectal (CCR) se encuentra entre los 5 tipos de cáncer con mayor incidencia a nivel mundial. Alrededor del 20% de los casos son diagnosticados en estadios metastásico, donde el tratamiento inicialmente era quimioterapia con una supervivencia global a 5 años de 12 a 14 meses. Es así que se investiga el papel de la angiogénesis tumoral, orientado al desarrollo de terapias, implementando su uso en estadios avanzados. Metodología: Se realizó una búsqueda sistemática en las bases de datos Embase, PubMed, SciELO y LILIACS con términos estandarizados a través de la herramienta MeSH y DECS bajo los lineamientos establecidos en las guías de revisiones sistemáticas y meta-análisis (Manual Cochrane). Se tomaron estudios clínicos aleatorizados controlados con pacientes con CCR metastásico, que hayan recibido quimioterapia sola o combinada con terapias antiangiogénicas, publicados en inglés y español entre el 2003 y 2013. Resultados: 6 artículos cumplieron con criterios de inclusión. Estos reportaron 15.8 meses en promedio de supervivencia global en el tratamiento de quimioterapia asociada a terapias biológicas frente a 14.4 meses con solo quimioterapia. Los eventos adversos de tipo vascular aumentaron más en el grupo de antiangiogénicos, reportando muertes debidas a perforaciones intestinales. Conclusiones: Los regímenes de quimioterapia asociadas a terapias antiangiogénicas brindan una mayor supervivencia global y libre de progresión, al igual que mayor número de tasas de respuesta. Son terapias con eventos adversos importantes pero que deberá seleccionarse bien al paciente para disminuir su riesgo de eventos. Palabras claves: Cáncer colorrectal metastásico, terapia anti-angiogénica, quimioterapia en segunda línea, receptor del factor de crecimiento de endotelio vascular, supervivencia global., Introduction: Colorectal cancer (CRC) is among the 5 types of cancer with the highest incidence worldwide. About 20% of cases are diagnosed in where the treatment was initially chemotherapy with an overall 5-year survival of 12 to 14 months metastatic stages. Thus the role of tumor angiogenesis therapies aimed at developing, implementing use in advanced stages is investigated. Methodology: A systematic search of the databases Embase, PubMed, SciELO and Liliacs data with standardized terms through the MeSH and DECS tool under the guidelines established in the guidelines of systematic reviews and meta-analyzes (Cochrane Manual) Revisions were made. randomized controlled trials were taken with patients with metastatic RCC who have received chemotherapy alone or combined with antiangiogenic therapies, published in English and Spanish between 2003 and 2013. Results: 6 articles met inclusion criteria. These reported 15.8 months median overall survival in the treatment of chemotherapy-associated biological therapies vs. 14.4 months with chemotherapy alone. Adverse vascular events increased more in the group of anti-angiogenic, reporting deaths due to intestinal perforations. Conclusions: chemotherapy regimens associated with antiangiogenic therapies provide greater overall and progression-free survival, as well as greater number of response rates. They are therapies with significant adverse events but to be selected either the patient to reduce their risk of events., Universidad del Rosario

Published
2016

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