Your search keyword '"Ionescu,Calin"' showing total 20 results

1. The extracellular matrix alteration, implication in modulation of drug resistance mechanism: friends or foes?

Author

Jurj, Ancuta, Ionescu, Calin, Berindan-Neagoe, Ioana, and Braicu, Cornelia

Published

2022

2. Global variation in the long-term outcomes of ypT0 rectal cancers

Author

Terrenato, Irene, Shinde, Rajesh S., Saklani, Avanish, Martins, Pedro, Videira, José Flávio, Bonci, Eduard-Alexandru, Achimas-Cadariu, Patriciu, Marinello, Franco, Espin, Eloy, Xenaki, Sofia, Lasithiotakis, Konstantinos, Rega, Daniela, Delrio, Paolo, Andrási, László, Lázár, György, Quattromani, Roberto, Elmore, Ugo, Branciforte, Martina Azzurra, Piazza, Diego, Sztipits, Tamás, Mersich, Tamás, Vigorita, Vincenzo, Ildefonso, Alberto San, Cianflocca, Desiree, Giuffrida, Maria Carmela, Biondi, Alberto, Persiani, Roberto, Košir, Jurij Aleš, Grosek, Jan, Rizzo, Gianluca, Coco, Claudio, Dieninyte-Misiune, Egle, Bausys, Rimantas, Bausys, Augustinas, Poskus, Tomas, Dupré, Aurélien, Muresan, Mihai-Stefan, Ionescu, Călin, Alyami, Mohammad, Cotte, Eddy, Candido, Francesca Di, Spinelli, Antonino, Lucarini, Alessio, Balducci, Genoveffa, Kisielewski, Michał, Pędziwiatr, Michał, Kroon, Hidde, Sammour, Tarik, Unger, Lukas, Stift, Anton, Marsanic, Patrizia, Muratore, Andrea, Uzunoglu, Mustafa Yener, Altintoprak, Fatih, Capponi, Michela Giulii, Poiasina, Elia, Brandl, Andreas, Aigner, Felix, Aparício, David, Leichsenring, Carlos, Corleone, Pio, Manzini, Nicolò de, Kabata, Paweł, Świerblewski, Maciej, Gallo, Gaetano, Trompetto, Mario, Negoi, Ionut, Beuran, Mircea, Souriti, Ahmad, Taylor, Gregory, De Luca, Raffaele, Simone, Michele, Bedford, Matthew, Charalampakis, Vasileios, Rajan, Shiv, Chaturvedi, Arun, Veltri, Marco, Parini, Dario, Turati, Luca, Sgroi, Giovanni, Bratu, Matei, Diaconescu, Bogdan, Slavchev, Mihail, Belev, Nikolay, Perfumo, Mariana Matzner, Rotholtz, Nicolas, Wajda, Justyna, Wysocki, Wojciech, Fernandez, Carmen Cagigas, Ruiz, Marcos Gomez, Marino, Serafino, Resta, Giuseppe, Ivanov, Tsvetomir, Dimitrov, Dobromir, Kaufmann, Claudia, Kafka-Ritsch, Reinhold, Yalkin, Omer, Ünal, Ali Ekrem, Loche, Giovanni Augusto, Cillara, Nicola, Colombo, Francesco, Foschi, Diego, Pollesel, Sara, Roviello, Franco, Lorenzon, Laura, Evrard, Serge, Beets, Geerard, Gonzalez-Moreno, Santiago, Kovacs, Tibor, D’Ugo, Domenico, and Polom, Karol

Published

2020

3. Nanoscale delivery systems for microRNAs in cancer therapy

Author

Boca, Sanda, Gulei, Diana, Zimta, Alina-Andreea, Onaciu, Anca, Magdo, Lorand, Tigu, Adrian Bogdan, Ionescu, Calin, Irimie, Alexandru, Buiga, Rares, and Berindan-Neagoe, Ioana

Published

2020

4. The silent healer: miR-205-5p up-regulation inhibits epithelial to mesenchymal transition in colon cancer cells by indirectly up-regulating E-cadherin expression

Author

Gulei, Diana, Magdo, Lorand, Jurj, Ancuta, Raduly, Lajos, Cojocneanu-Petric, Roxana, Moldovan, Alin, Moldovan, Cristian, Florea, Adrian, Pasca, Sergiu, Pop, Laura-Ancuta, Moisoiu, Vlad, Budisan, Liviuta, Pop-Bica, Cecilia, Ciocan, Cristina, Buiga, Rares, Muresan, Mihai-Stefan, Stiufiuc, Rares, Ionescu, Calin, and Berindan-Neagoe, Ioana

Published

2018

5. The clinical and biological significance of MIR-224 expression in colorectal cancer metastasis

Author

Ling, Hui, Pickard, Karen, Ivan, Cristina, Isella, Claudio, Ikuo, Mariko, Mitter, Richard, Spizzo, Riccardo, Bullock, Marc D, Braicu, Cornelia, Pileczki, Valentina, Vincent, Kimberly, Pichler, Martin, Stiegelbauer, Verena, Hoefler, Gerald, Almeida, Maria I, Hsiao, Annie, Zhang, Xinna, Primrose, John N, Packham, Graham K, Liu, Kevin, Bojja, Krishna, Gafà, Roberta, Xiao, Lianchun, Rossi, Simona, Song, Jian H, Vannini, Ivan, Fanini, Francesca, Kopetz, Scott, Zweidler-McKay, Patrick, Wang, Xuemei, Ionescu, Calin, Irimie, Alexandru, Fabbri, Muller, Lanza, Giovanni, Hamilton, Stanley R, Berindan-Neagoe, Ioana, Medico, Enzo, Mirnezami, Alex H, Calin, George A, and Nicoloso, Milena S

Published

2016

6. Spontaneous Intramural Duodenal Hematoma - A Rare Entity.

Author

Iliescu, Laura Elena, Grumeza, Mihaela, Stanciu, Adriana Mercan, Toma, Letitia, Zgura, Anca, Cristian, Popescu Gabriel, Ionescu, Calin, and Bacinschi, Xenia

Published

2022

7. Circulating microRNA-194 and microRNA-1228 Could Predict Colon Cancer Proliferation via Phospho S6 Modulation.

Author

Pasca, Sergiu, Ionescu, Calin, Andras, David, Eniu, Dan, Mureșan, Mihai-Andrei, Magdo, Lorand, Jurj, Ancuta, Raduly, Lajos, Cojocneanu, Roxana, Petrushev, Bobe, Zaharie, Florin, Irimie, Alexandru, Berindan-Neagoe, Ioana, and Muresan, Mihai-Stefan

Subjects

*COLON cancer, *MICRORNA, *WESTERN immunoblotting, *CELL lines

Abstract

Background & Aims: Although colon cancer has a decreasing incidence trend in Europe, because of its still high frequency and not fully understood pathogenesis, this malignancy still remains a subject of intense research. The aim of this study was to investigate the role of microRNA-194 and microRNA-1228 in colon cancer proliferation. Methods: RNA was extracted from patients with colon cancer with or without advanced disease and microRNA expression levels were determined through qRT-PCR. Assays were performed on HCT116 cell line and included qRT-PCR, western blotting and cell counting. Results: We observed that both microRNAs 194 and 1228 were altered in patients with colon cancer compared with healthy individuals. We observed a lower expression of both microRNA-194 and microRNA-1228 in patients with advanced colon cancer. To validate their pathogenetic role we performed viability and invasion assays on HCT116 cell line transfected with mimics or inhibitors of the mentioned microRNAs, with observable changes in viability and invasion. Furthermore, to determine the altered signaling induced by these microRNAs, we performed western blotting for phospho S6 on HCT116 cells transfected with mimic and inhibitor of the above-mentioned microRNAs with observable differences. Conclusion: In the current study we have shown that both microRNA-194 and microRNA-1228 alteration was correlated with the presence of advanced colon cancer, a fact that was further validated in vitro through an invasion assay. Moreover, we have also shown that their effect might be mediated through phospho S6 expression. [ABSTRACT FROM AUTHOR]

Published

2020

8. Critical function of circular RNAs in lung cancer.

Author

Drula, Rares, Braicu, Cornelia, Harangus, Antonia, Nabavi, Seyed M., Trif, Monica, Slaby, Ondrej, Ionescu, Calin, Irimie, Alexandru, and Berindan‐Neagoe, Ioana

Published

2020

9. An Emerging Class of Long Non-coding RNA With Oncogenic Role Arises From the snoRNA Host Genes.

Author

Zimta, Alina-Andreea, Tigu, Adrian Bogdan, Braicu, Cornelia, Stefan, Cristina, Ionescu, Calin, and Berindan-Neagoe, Ioana

Subjects

NON-coding RNA, SMALL interfering RNA, GENES, PLANT gene silencing, CELL cycle, METASTASIS

Abstract

The small nucleolar RNA host genes (SNHGs) are a group of long non-coding RNAs, which are reported in many studies as being overexpressed in various cancers. With very few exceptions, the SNHGs (SNHG1, SNHG3, SNHG5, SNHG6, SNHG7, SNHG12, SNHG15, SNHG16, SNHG20) are recognized as inducing increased proliferation, cell cycle progression, invasion, and metastasis of cancer cells, which makes this class of transcripts a viable biomarker for cancer development and aggressiveness. Through our literature research, we also found that silencing of SNHGs through small interfering RNAs or short hairpin RNAs is very effective in both in vitro and in vivo experiments by lowering the aggressiveness of solid cancers. The knockdown of SNHG as a new cancer therapeutic option should be investigated more in the future. [ABSTRACT FROM AUTHOR]

Published

2020

10. SERS-based differential diagnosis between multiple solid malignancies: breast, colorectal, lung, ovarian and oral cancer.

Author

Moisoiu, Vlad, Stefancu, Andrei, Gulei, Diana, Boitor, Radu, Magdo, Lorand, Raduly, Lajos, Pasca, Sergiu, Kubelac, Paul, Mehterov, Nikolay, Chiș, Vasile, Simon, Marioara, Muresan, Mihai, Irimie, Alexandra Iulia, Baciut, Mihaela, Stiufiuc, Rares, Pavel, Ioana E, Achimas-Cadariu, Patriciu, Ionescu, Calin, Lazar, Vladimir, and Sarafian, Victoria

Published

2019

11. Exosomes at a glance - common nominators for cancer hallmarks and novel diagnosis tools.

Author

Gulei, Diana, Petrut, Bogdan, Tigu, Adrian Bogdan, Onaciu, Anca, Fischer-Fodor, Eva, Atanasov, Atanas G., Ionescu, Calin, and Berindan-Neagoe, Ioana

Subjects

MELANOMA, PATHOLOGICAL anatomy, CELL proliferation, MESENCHYMAL stem cells, CANCER cells

Abstract

Cancer represents a heterogeneous disease with multiple levels of regulation and a dynamic environment that sustains the evolution of the malignant mass. This dynamic is in part sustained by a class of extracellular vesicles termed exosomes that are able to imprint the pathological state by incorporating differential cargos in order to facilitate cell-to-cell communication. Exosomes are stable within the extracellular medium and function as shuttles secreted by healthy or pathological cells, being further taken by the accepting cell with direct effects on its phenotype. The exosomal trafficking is deeply involved in multiple levels of cancer development with roles in all cancer hallmarks. Nowadays, studies are constantly exploring the ability of exosomes to sustain the malignant progression in order to attack this pathological trafficking and impair the ability of the tumor mass to expand within the organisms. As important, the circulatory characteristics of exosomes represent a steady advantage regarding the possibility of using them as minimally invasive diagnosis tools, where cancer patients’ present modified exosomal profiles compared to the healthy ones. This last characteristic, as novel diagnosis tools, has the advantage of a possible rapid transition within the clinic, compared to the studies that evaluate the therapeutic meaning. [ABSTRACT FROM AUTHOR]

Published

2018

12. TIMP-1 Expression in Human Colorectal Cancer Is Associated with SMAD3 Gene Expression Levels: A Pilot Study.

Author

Ionescu, Calin, Braicu, Cornelia, Chiorean, Roxana, Petrie, Roxana Cojocneanu, Neagoe, Emilian, Pop, Laura, Chira, Sergiu, and Berindan-Neagoe, Ioana

Subjects

*GENE expression, *METALLOPROTEINASES, *COLON cancer prognosis, *SMAD proteins, *POLYMERASE chain reaction

Abstract

Background & Aims: The prognosis of colorectal cancer (CRC) varies considerably, and there is a compelling need to identify novel biomarkers with prognostic significance. The aim of the present study was to evaluate the prognostic value of a panel of six genes (CDH1, SMAD3, TGFfil, ICAM-1, TIMP-1 and MUC12) in CRC patients. Methods: We evaluated these genes by qRT-PCR in normal and CRC tumor tissue, and correlated the relative gene expression values with clinical, pathological aspects and other biological factors. Results: RNA expression levels of CDH1, SMAD3, TGFfil, ICAM-1, TIMP-1 and MUC12 were measured by qRT-PCR in a set of 39 tumor samples and non-cancer tissue. Statistically significant increases in expression levels were found for ICAM-1 and TIMP-1 when comparing tumor samples to the non-tumor group. Conclusions: Among the genes which displayed differential expressions between tumor tissue and adjoining normal tissue, the ones that presented statistically significant correlations were TIMP-1 and SMAD3, possibly with prognostic significance. [ABSTRACT FROM AUTHOR]

Published

2014

13. Epithelial–Mesenchymal Transition Gene Signature Related to Prognostic in Colon Adenocarcinoma.

Author

Busuioc, Constantin, Ciocan-Cartita, Cristina Alexandra, Braicu, Cornelia, Zanoaga, Oana, Raduly, Lajos, Trif, Monica, Muresan, Mihai-Stefan, Ionescu, Calin, Stefan, Cristina, Crivii, Carmen, Al Hajjar, Nadim, Mǎrgǎrit, Simona, and Berindan-Neagoe, Ioana

Subjects

EPITHELIAL-mesenchymal transition, COLON (Anatomy), ADENOCARCINOMA, PHENOTYPES, GENES

Abstract

Colon adenocarcinoma (COAD) remains an important cause of cancer-related mortality worldwide. Epithelial–mesenchymal transition (EMT) is a key mechanism, promoting not only the invasive or metastatic phenotype but also resistance to therapy. Using bioinformatics approaches, we studied the alteration on EMT related genes and its implication on COAD prognostic based on public datasets. For the EMT mechanisms, two overexpressed genes were identified (NOX4 and IGF2BP3), as well as five downregulated genes (BMP5, DACT3, EEF1A2, GCNT2 and SFRP1) that were related to prognosis in COAD. A qRT-PCR validation step was conducted in a COAD patient cohort comprising of 29 tumor tissues and 29 normal adjacent tissues, endorsing the expression level for BMP5, as well as for two of the miRNAs targeting key EMT related genes, revealing upregulation of miR-27a-5p and miR-146a-5p. The EMT signature can be used to develop a panel of biomarkers for recurrence prediction in COAD patients, which may contribute to the improvement of risk stratification for the patients. [ABSTRACT FROM AUTHOR]

Published

2021

14. Hsa-miR-125b Therapeutic Role in Colon Cancer Is Dependent on the Mutation Status of the TP53 Gene.

Author

Cenariu, Diana, Zimta, Alina-Andreea, Munteanu, Raluca, Onaciu, Anca, Moldovan, Cristian Silviu, Jurj, Ancuta, Raduly, Lajos, Moldovan, Alin, Florea, Adrian, Budisan, Liviuta, Pop, Laura Ancuta, Magdo, Lorand, Albu, Mihai Tudor, Tonea, Rares Bogdan, Muresan, Mihai-Stefan, Ionescu, Calin, Petrut, Bogdan, Buiga, Rares, Irimie, Alexandru, and Gulei, Diana

Subjects

COLON cancer, CANCER cells, COLORECTAL cancer, DISEASE progression, PHENOTYPES

Abstract

Colon cancer is the third most common cancer type worldwide and is highly dependent on DNA mutations that progressively appear and accumulate in the normal colon epithelium. Mutations in the TP53 gene appear in approximately half of these patients and have significant implications in disease progression and response to therapy. miR-125b-5p is a controversial microRNA with a dual role in cancer that has been reported to target specifically TP53 in colon adenocarcinomas. Our study investigated the differential therapeutic effect of miR-125b-5p replacement in colon cancer based on the TP53 mutation status of colon cancer cell lines. In TP53 mutated models, miR-125b-5p overexpression slows cancer cells' malignant behavior by inhibiting the invasion/migration and colony formation capacity via direct downregulation of mutated TP53. In TP53 wild type cells, the exogenous modulation of miR-125b-5p did not significantly affect the molecular and phenotypic profile. In conclusion, our data show that miR-125b-5p has an anti-cancer effect only in TP53 mutated colon cancer cells, explaining partially the dual behavior of this microRNA in malignant pathologies. [ABSTRACT FROM AUTHOR]

Published

2021

15. Plasma and Tissue Specific miRNA Expression Pattern and Functional Analysis Associated to Colorectal Cancer Patients.

Author

Cojocneanu, Roxana, Braicu, Cornelia, Raduly, Lajos, Jurj, Ancuta, Zanoaga, Oana, Magdo, Lorand, Irimie, Alexandru, Muresan, Mihai-Stefan, Ionescu, Calin, Grigorescu, Mircea, and Berindan-Neagoe, Ioana

Subjects

TISSUE analysis, CARCINOGENESIS, BIOMARKERS, BLOOD plasma, CANCER chemotherapy, CANCER patients, COLON tumors, FLUIDS, GENE expression, LONGITUDINAL method, METABOLISM, POLYMERASE chain reaction, RECTUM tumors, TRANSCRIPTION factors, MICROARRAY technology, MICRORNA

Abstract

An increasing number of studies suggest the implication of microRNAs (miRNAs) in colorectal (CRC) carcinogenesis and disease progression. Nevertheless, the basic mechanism is not yet clear. We determined plasma miRNA expression levels using Agilent microarray technology followed by overlapping with The Cancer Genome Atlas (TCGA) tissue data and a qRT-PCR validation step and analysis of the altered miRNA signatures to emphasize new mechanistic insights. For TGCA dataset, we identified 156 altered miRNAs (79 downregulated and 77 upregulated) in colorectal tissue samples versus normal tissue. The microarray experiment is based on 16 control samples, 38 CRC plasma samples from colorectal cancer patients who have not undergone chemotherapy, and 17 chemo-treated samples. In the case of the analysis of CRC cancer versus healthy control we identified 359 altered miRNAs (214 downregulated and 60 upregulated), considering as the cutoff value a fold-change of ±1.5 and p < 0.01. An additional microarray analysis was performed on plasma from untreated colorectal cancer (n = 38) and chemotherapy-treated colorectal cancer patients (n = 17), which revealed 15 downregulated miRNAs and 53 upregulated miRNAs, demonstrating that the plasma miRNA pattern is affected by chemotherapy and emphasizing important regulators of drug resistance mechanisms. For the validation of the microarray data, we selected a panel of 4 miRNAs from the common miRNA signatures for colon and rectal cancer (miR-642b-3p, miR-195-5p and miR-4741). At the tissue level, the expression levels were in agreement with those observed in colorectal plasma. miR-1228-3p, the top upregulated miRNA in CRC, was chosen to be validated on tissue and plasma samples, as it was demonstrated to be downregulated at tissue level in our patient cohort. This was confirmed by TCGA data and was one example of ta ranscript that has a different expression level between tumor tissue and plasma. Developing more efficient investigation methods will help explain the mechanisms responsible for miRNAs released in biofluids, which is the most upregulated transcript in colorectal plasma samples and which can function as a prediction tool within the oncological field. [ABSTRACT FROM AUTHOR]

Published

2020

16. Inhibitory Effect of CAPE and Kaempferol in Colon Cancer Cell Lines—Possible Implications in New Therapeutic Strategies.

Author

Budisan, Liviuta, Gulei, Diana, Jurj, Ancuta, Braicu, Cornelia, Zanoaga, Oana, Cojocneanu, Roxana, Pop, Laura, Raduly, Lajos, Barbat, Alexandru, Moldovan, Alin, Moldovan, Cristian, Tigu, Adrian Bogdan, Ionescu, Calin, Atanasov, Atanas G., Irimie, Alexandru, and Berindan-Neagoe, Ioana

Subjects

CANCER cells, CELL lines, CAFFEIC acid, CELL motility, APOPTOSIS

Abstract

Background: Phytochemicals are natural compounds synthesized as secondary metabolites in plants and represent an important source of molecules with therapeutic applications. Attention is accorded to their potential in anti-cancer therapies as single agents or adjuvant treatment. Herby, we evaluated the in vitro effects of a panel of natural compounds with focus on caffeic acid phenethyl ester (CAPE) and Kaempferol for the treatment of human colon cancer. Methods: We exposed two human colon cancer cell lines, RKO and HCT-116, followed by functional examination of cell viability, cell proliferation and invasion, cell cycle, apoptosis, and autophagy. Modifications in gene expression were investigated through microarray and detection of existing mutations and finding of new ones was done with the help of Next Generation Sequencing (NGS). Results: Both CAPE and Kaempferol inhibit cell proliferation, motility and invasion, and stimulate apoptosis and autophagy, concomitant with modifications in coding and noncoding genes' expression. Moreover, there are pathogenic mutations that are no longer found upon treatment with CAPE and Kaempferol. Conclusions: Our findings indicate that CAPE and Kaempferol have the ability to negatively influence the development and advancement of colon cancer in vitro by specifically altering the cells at the molecular level; this activity can be exploited in possible adjuvant therapies once the optimal dose concentration with minimal side effects but with cancer inhibitory activity is set in vivo. [ABSTRACT FROM AUTHOR]

Published

2019

17. A Comprehensive Review on MAPK: A Promising Therapeutic Target in Cancer.

Author

Braicu C, Buse M, Busuioc C, Drula R, Gulei D, Raduly L, Rusu A, Irimie A, Atanasov AG, Slaby O, Ionescu C, and Berindan-Neagoe I

Abstract

The mitogen-activated protein kinase (MAPK) pathway is an important bridge in the switch from extracellular signals to intracellular responses. Alterations of signaling cascades are found in various diseases, including cancer, as a result of genetic and epigenetic changes. Numerous studies focused on both the homeostatic and the pathologic conduct of MAPK signaling; however, there is still much to be deciphered in terms of regulation and action models in both preclinical and clinical research. MAPK has implications in the response to cancer therapy, particularly the activation of the compensatory pathways in response to experimental MAPK inhibition. The present paper discusses new insights into MAPK as a complex cell signaling pathway with roles in the sustenance of cellular normal conduit, response to cancer therapy, and activation of compensatory pathways. Unfortunately, most MAPK inhibitors trigger resistance due to the activation of compensatory feed-back loops in tumor cells and tumor microenvironment components. Therefore, novel combinatorial therapies have to be implemented for cancer management in order to restrict the possibility of alternative pathway activation, as a perspective for developing novel therapies based on integration in translational studies., Competing Interests: The authors have no conflicts of interest to declare.

Published

2019

18. SIRT1 in the Development and Treatment of Hepatocellular Carcinoma.

Author

Farcas M, Gavrea AA, Gulei D, Ionescu C, Irimie A, Catana CS, and Berindan-Neagoe I

Abstract

Hepatocellular carcinoma (HCC) is one of the most common causes of cancer-related death worldwide. Current treatment options for inoperable HCCs have decreased therapeutic efficacy and are associated with systemic toxicity and chemoresistance. Sirtuin 1 (SIRT1) is a nicotinamide adenine dinucleotide-dependent enzyme that is frequently overexpressed in HCC, where it promotes tumorigenicity, metastasis, and chemoresistance. SIRT1 also maintains the tumorigenic and self-renewal proprieties of liver cancer stem cells. Multiple tumor-suppressive microRNAs (miRNAs) are downregulated in HCC and, as a consequence, permit SIRT1-induced tumorigenicity. However, either directly targeting SIRT1, combining conventional chemotherapy with SIRT1 inhibitors, or upregulating tumor-suppressive miRNAs may improve therapeutic efficacy and patient outcomes. Here, we present the interaction between SIRT1, miRNAs, and liver cancer stem cells and discuss the consequences of their interplay for the development and treatment of HCC., (Copyright © 2019 Farcas, Gavrea, Gulei, Ionescu, Irimie, Catana and Berindan-Neagoe.)

Published

2019

19. Premature senescence activation in DLD-1 colorectal cancer cells through adjuvant therapy to induce a miRNA profile modulating cellular death.

Author

Chira S, Raduly L, Braicu C, Jurj A, Cojocneanu-Petric R, Pop L, Pileczki V, Ionescu C, and Berindan-Neagoe I

Abstract

Cancer, and particularly colon cancer, is associated with an increasing number of cases resistant to chemotherapy. One approach to overcome this, and to improve the prognosis and outcome of patients, is the use of adjuvant therapy alongside the standard chemotherapy regiment. In the present study, the effect of deuterium-depleted water (DDW) as a potential modulator of adjuvant therapy on DLD-1 colorectal cancer models was assessed. A number of functionality assays were performed, including MTT, apoptosis and autophagy, and mitochondrial activity and senescence assays, in addition to assessing the capacity to modify the pattern of released miRNA via microarray technology. No significant effect on cell viability was identified, but an increase in mitochondrial activity and a weak pro-apoptotic effect were observed in the treated DLD-1 cells cultured in DDW-prepared medium compared with those grown in standard conditions (SC). Furthermore, the findings revealed the capacity of DDW medium to promote senescence to a higher degree compared with SC. The exosome-released miRNA pattern was significantly modified for the cells maintained in DDW compared with those maintained in SC. These findings suggest that DDW may serve as an adjuvant treatment; however, a better understanding of the underlying molecular mechanism of action will be useful for developing novel and efficient therapeutic strategies, in which the transcriptomic pattern serves an important role.

Published

2018

20. The venous thrombosis of the pancreatic graft.

Author

Ionescu C, Wolf P, Ellero B, and Mihaescu G

Subjects

Adolescent, Adult, Diabetes Mellitus, Type 1 surgery, Female, Follow-Up Studies, Humans, Immunosuppression Therapy, Kidney Transplantation, Male, Middle Aged, Monitoring, Physiologic, Postoperative Care, Recurrence, Replantation, Risk Factors, Time Factors, Tissue Donors, Ultrasonography, Doppler, Pulsed, Graft Occlusion, Vascular, Iliac Vein, Pancreas Transplantation adverse effects, Portal Vein, Venous Thrombosis diagnostic imaging, Venous Thrombosis prevention & control

Abstract

Background and Aims: Venous thrombosis of the pancreatic graft is the main nonimmunological cause of the loss of transplants. It has a frequency between 0.8 to 20% according to literature. In this study our team tried to identify the risk factors related to the donor, the recipient including the surgical techniques involved., Methods: The study was conducted in the Department of Transplant Surgery, University Hospital Strasbourg-Hautepierre. 37 patients, with type I diabetes who had been submitted to 7 transplantations of segmentary pancreas and 30 of total pancreas and kidney during 09.07.1992 and 14.08.2006 were included in the study. The surgery comprised the retroperitoneal placement of the pancreas and kidney and the anastomosis with the urinary bladder., Results: In the immediate evolution we observed 4 thromboses (10.5%). All 4 thromboses were in the group of kidney and total pancreas transplantations. Two of these 4 patients were retransplanted and presented recurrence of thrombosis at 17 days and 1 year., Conclusions: To prevent thrombosis, it is necessary to perform surgery which avoids unnecessary handling and which ensures broad, tension free vascular anastomoses. The method of early monitoring by pulsed Doppler related to the biological data and the clinical state are suggestive to diagnose thrombosis. The venous thrombosis of the graft implies pancreatic explantation. Retransplantation in patients who have undergone thrombosis of the graft is possible only in well selected patients.

Published

2007