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2. Hepatocellular adenomas with severe intra-abdominal bleeding, related to an underlying coagulation disorder:a case report

Author

Oudmaijer, C. A.J., Sprakel, J., Sprengers, D., Wiese, K. A., Tintel, N. Vogelaar, Franken, J. I., Terkivatan, T., Porte, R. J., IJzermans, J. N.M., Oudmaijer, C. A.J., Sprakel, J., Sprengers, D., Wiese, K. A., Tintel, N. Vogelaar, Franken, J. I., Terkivatan, T., Porte, R. J., and IJzermans, J. N.M.

Abstract

Background: Hepatocellular adenoma is a rare benign liver tumor. Typically, hepatocellular adenomas are solitary and are found in young women who use estrogen-containing contraceptives. The occurrence of multiple hepatocellular adenoma has been linked to higher body mass index, and as the prevalence of overweight increases, multiple hepatocellular adenomas are seen more often. An hepatocellular adenoma does not always necessitate treatment, as they can regress under conservative strategies. In incidental cases, an adenoma presents owing to bleeding, which is mostly self-limiting. If it is not, embolization of hepatic involved vessels is indicated. Case presentation: In this case report, we discuss a 42-year old Caucasian woman with multiple hepatocellular bleeds, treated by multiple endovascular procedures. After the first embolization of an adenoma in the right liver lobe, a second bleed occurred in the left lobe, necessitating additional endovascular intervention. During admittance, treatment was complicated by pulmonary embolism and a pneumonia. During follow-up, our patient was diagnosed with antiphospholipid syndrome. Conclusion: Hepatocellular adenoma is a rare diagnosis that requires centralized expertise. This particular case illustrates the complexity of treatment strategies for associated intra-abdominal bleeding and possible complications. Although liver adenoma is often an incidental finding, it can also result in significant morbidity. Centralization of treatment leads to expertise in managing complex treatment strategies.

Published
2024

3. Transarterial Chemoembolization With Drug-Eluting Beads Versus Stereotactic Body Radiation Therapy for Hepatocellular Carcinoma: Outcomes From a Multicenter, Randomized, Phase 2 Trial (the TRENDY Trial).

Author

Méndez Romero, A., Holt, B. van der, Willemssen, F.E.J.A., Man, R.A. de, Heijmen, B.J.M., Habraken, S., Westerveld, H., Delden, O.M. van, Klümpen, H.J., Tjwa, E.T., Braam, P.M., Jenniskens, S.F.M., Vanwolleghem, T., Weytjens, R., d'Archambeau, O., Vos-Geelen, J. de, Buijsen, J., Leij, C. van der, Toom, W. den, Sprengers, D., Ijzermans, J.N.M., Moelker, A., Méndez Romero, A., Holt, B. van der, Willemssen, F.E.J.A., Man, R.A. de, Heijmen, B.J.M., Habraken, S., Westerveld, H., Delden, O.M. van, Klümpen, H.J., Tjwa, E.T., Braam, P.M., Jenniskens, S.F.M., Vanwolleghem, T., Weytjens, R., d'Archambeau, O., Vos-Geelen, J. de, Buijsen, J., Leij, C. van der, Toom, W. den, Sprengers, D., Ijzermans, J.N.M., and Moelker, A.

Abstract

Contains fulltext : 296077.pdf (Publisher’s version ) (Open Access), PURPOSE: To compare transarterial chemoembolization delivered with drug eluting beads (TACE-DEB) with stereotactioc body radiation therapy (SBRT) in patients with hepatocellular carcinoma (HCC) in a multicenter randomized trial. METHODS AND MATERIALS: Patients were included if they were eligible for TACE. They could also be recruited if they required treatment prior to liver transplantation. A maximum of four TACE-DEB procedures and ablation after incomplete TACE-DEB were both allowed. SBRT was delivered in six fractions of 8-9Gy. Primary end point was time to progression (TTP). Secondary endpoints were local control (LC), overall survival (OS), response rate (RR), toxicity, and quality of life (QoL). The calculated sample size was 100 patients. RESULTS: Between May 2015 and April 2020, 30 patients were randomized to the study. Due to slow accrual the trial was closed prematurely. Two patients in the SBRT arm were considered ineligible leaving 16 patients in the TACE-DEB arm and 12 in the SBRT arm. Median follow-up was 28.1 months. Median TTP was 12 months for TACEDEB and 19 months for SBRT (p=0.15). Median LC was 12 months for TACE-DEB and >40 months (not reached) for SBRT (p=0.075). Median OS was 36.8 months for TACEDEB and 44.1 months for SBRT (p=0.36). A post-hoc analysis showed 100% for SBRT 1- and 2-year LC, and 54.4% and 43.6% for TACE-DEB (p=0.019). Both treatments resulted in RR>80%. Three episodes of possibly related toxicity grade ≥3 were observed after TACE-DEB. No episodes were observed after SBRT. QoL remained stable after both treatment arms. CONCLUSIONS: In this trial, TTP after TACE-DEB was not significantly improved by SBRT, while SBRT showed higher local antitumoral activity than TACE-DEB, without detrimental effects on OS, toxicity and QoL. To overcome poor accrual in randomized trials that include SBRT, and to generate evidence for including SBRT in treatment guidelines, international cooperation is needed.

Published
2023

7. Trends in incidence, diagnosis, treatment and survival of hepatocellular carcinoma in a low-incidence country

Author

Reinders, M.T.M., Meer, S. van, Burgmans, M.C., Jong, K.P. de, Klumpen, H.J., Man, R.A. de, Ramsoekh, D., Sprengers, D., Tjwa, E.T.T.L., Vos-Geelen, J. de, Erpecum, K.J. van, Geest, L.G.M. van der, Dutch Hepatocellular & Cholangioca, Interne Geneeskunde, MUMC+: MA Medische Oncologie (9), RS: GROW - R3 - Innovative Cancer Diagnostics & Therapy, Oncology, CCA - Cancer Treatment and Quality of Life, AGEM - Amsterdam Gastroenterology Endocrinology Metabolism, Gastroenterology & Hepatology, Gastroenterology and hepatology, Amsterdam Gastroenterology Endocrinology Metabolism, Groningen Institute for Organ Transplantation (GIOT), and Guided Treatment in Optimal Selected Cancer Patients (GUTS)

Subjects
Data Analysis, Male, 0301 basic medicine, Cancer Research, medicine.medical_specialty, Carcinoma, Hepatocellular, Survival, Hepatocellular carcinoma, medicine.medical_treatment, Liver transplantation, History, 21st Century, Gastroenterology, Cancer diagnostics, 03 medical and health sciences, All institutes and research themes of the Radboud University Medical Center, 0302 clinical medicine, Case mix index, SDG 3 - Good Health and Well-being, Internal medicine, Biopsy, medicine, MANAGEMENT, Humans, Aged, Netherlands, medicine.diagnostic_test, business.industry, Incidence, Incidence (epidemiology), Liver Neoplasms, Middle Aged, Ablation, medicine.disease, Cancer registry, Renal disorders Radboud Institute for Molecular Life Sciences [Radboudumc 11], 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Cancer treatment, VOLUME, Female, Liver cancer, business
Abstract

Objective: Evaluation of the trends in incidence, diagnostics, treatment and survival of patients with hepatocellular carcinoma (HCC) in the Netherlands.Method: Data regarding incidence, diagnostics, primary treatment and survival of patients with HCC in the period 2009-2016 were obtained from the Netherlands Cancer Registry. Trends in incidence, diagnostics, various treatment modalities (except liver transplantation, due to inaccurate data) and regional treatment preferences were analysed. Survival was evaluated using Kaplan-Meier curves and multivariable Cox proportional hazard regression modelling.Results: In the period of 2009-2016, 3838 patients were diagnosed with HCC. A distinct decrease in the percentage of patients who underwent tumour biopsy was observed (from 51% in 2009-2010 to 42% in 2015-2016). Percentage of patients who underwent cancer treatment increased markedly (from 49% in 2009-2010 to 57% in 2015-2016), mainly because of an increasing use of resection and ablation. The number of hospitals where resections were performed or sorafenib treatment prescribed decreased slightly. The number of hospitals sporadically (

Published
2020
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9. Stereotactic Body Radiation Therapy Following Chemotherapy for Unresectable Perihilar Cholangiocarcinoma: The STRONG Trial, a Phase I Feasibility Study

Author

Baak, R., primary, Willemssen, F.E.J.A., additional, van Norden, Y., additional, Milder, M., additional, Heijmen, B.J.M., additional, Eskens, F.A.L.M., additional, Koerkamp, B. Groot, additional, Sprengers, D., additional, van Driel, L.M.J.W., additional, Klümpen, H.J., additional, den Toom, W., additional, Koedijk, M.S., additional, and Romero, A. Mendez, additional

Published
2021
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11. Real-life data on the impact of successful downstaging in patients with hepatocellular carcinoma: A Dutch Multicenter Study

Author

Broekhoven, A.G.C., Fiocco, M., Sprengers, D., Takkenberg, R.B., Meer, S. van, Erpecum, K.J. van, Ramsoekh, D., Verspaget, H.W., Burgmans, M.C., Osanto, S., Baranski, A.G., Hoek, B. van, Coenraad, M.J., Gastroenterology and Hepatology, Amsterdam Gastroenterology Endocrinology Metabolism, Gastroenterology & Hepatology, and Gastroenterology and hepatology

Subjects
Science & Technology, Carcinoma, Hepatocellular, Hepatology, Hepatocellular carcinoma, Liver Neoplasms, LARGE COHORT, LIVER-TRANSPLANTATION, digestive system diseases, Medicine, General & Internal, Treatment Outcome, SDG 3 - Good Health and Well-being, Downstaging, General & Internal Medicine, Liver cirrhosis, Internal Medicine, Humans, Life Sciences & Biomedicine, Neoplasm Staging, Retrospective Studies, Cancer
Abstract

Patients with Barcelona Clinic Liver Cancer intermediate stage hepatocellular carcinoma (HCC) theoretically are an excellent group to consider downstaging using locoregional therapy (LRT) since they do not have extrahepatic spread or vascular invasion. Once successful, this can change the treatment strategy from palliative to curative intention. Although downstaging therapy is suggested in guidelines, it is still not widely accepted. Moreover, studies on downstaging are mainly performed in high-incidence HCC countries. Therefore, our aim was to gain insight in therapeutic strategies in patients with intermediate stage HCC and their impact on intention-to-treat survival in a real-life setting in a low-incidence HCC country. We retrospectively analyzed data from the national Dutch HCC registry. From this database, consisting of 1409 patients with a diagnosis of HCC between 2005-2013 in 5 Dutch tertiary referral centers, we identified 165 patients with intermediate stage HCC. Out of these patients, 63 (38%) were not offered LRT, whereas 102 (62%) did receive LRT. Subsequently, 50 (49%) of the 102 patients who received LRT were successfully downstaged. Eleven patients (22% of successfully downstaged patients) eventually underwent liver transplantation. Cox regression analysis showed that a lower MELD score, an AFP value

Published
2021
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12. 110 Poster - Do patients with breast cancer receive the optimal personalized follow up?

Author

van Middelkoop-van Hoeve, J., Ankersmid, J., Strobbe, L., Velting, M., Sprengers, D., Verloop, Janneke, Schrijer, R., Kistemaker, B., Siesling, S., and Health Technology & Services Research

Abstract

Background: The incidence of breast cancer has increased in the last 15 years. Due to improved survival, the 10-year prevalence has increased even more, resulting in more focus on the late effects of cancer treatment and survivorship. Good quality of follow up and aftercare means that late effects of treatment and disease can be prevented or signaled at an early stage and that patients receive tailored care. However, it is unclear how optimal and efficient follow up and aftercare should look like, from the patients perspective as well as the perspective of health care organizations.

Published
2020

14. Lactobacillus GG prevents recurrence of colitis in HLA-B27 transgenic rats after antibiotic treatment. (Inflammatory Bowel Disease)

Author

Dieleman, L.A., Goerres, M.S., Arends, A., Sprengers, D., Torrice, C., Hoentjen, F., Grenther, W.B., and Sartor, R.B.

Subjects
Prevention, Health aspects, Lactobacillus -- Health aspects, Colitis -- Prevention
Abstract

Background and aims: Bacteroides vulgatus induces colitis in gnotobiotic HLA- B27 transgenic (TG) rats while broad spectrum antibiotics prevent and treat colitis in specific pathogen free (SPF) TG rats although [...]

Published
2003

16. Stopping nucleos(t)ide analogue treatment in Caucasian hepatitis B patients after HBeAg seroconversion is associated with high relapse rates and fatal outcomes

Author

Van Hees, S., Bourgeois, S., Van Vlierberghe, H., Sersté, T., Francque, S., Michielsen, P., Sprengers, D., Reynaert, H., Henrion, J., Negrin Dastis, S., Delwaide, J., Lasser, L., Decaestecker, J., Orlent, H., Janssens, F., Robaeys, G., Colle, I., Stärkel, P., Moreno, C., Nevens, F., Vanwolleghem, T., Van Hees, Stijn, Bourgeois, Stefan, Van Vlierberghe, Hans, Sersté, Thomas, Francque, Sven, Michielsen, Peter, Sprengers, Dirk, Reynaert, Hendrik, Henrion, Jean, Negrin‐Dastis, Sergio, Delwaide, Jean, Lasser, Luc, Decaestecker, Jochen, Orlent, Hans, Janssens, Filip, Robaeys, Geert, Colle, Isabelle, Stärkel, Peter, Moreno, Christophe, Nevens, Frederik, Vanwolleghem, Thomas, Nuclear Medicine, Liver Cell Biology, Laboratory of Molecullar and Cellular Therapy, Basic (bio-) Medical Sciences, Faculty of Medicine and Pharmacy, Gastroenterology, Gastroenterology & Hepatology, and Belgian NA Stop Study Group

Subjects
Male, 0301 basic medicine, HBsAg, Antibodies, Viral, Gastroenterology, Cohort Studies, Fatal Outcome, 0302 clinical medicine, Recurrence, HEPATOCELLULAR-CARCINOMA, E-ANTIGEN, Medicine and Health Sciences, Pharmacology (medical), Hepatitis B e Antigens, ENTECAVIR TREATMENT, Pharmacology. Therapy, Nucleosides, Middle Aged, Hepatitis B, PREDICTS, Treatment Outcome, HBeAg, Seroconversion, Hepatocellular carcinoma, SUSTAINED VIROLOGICAL RESPONSE, Cohort, Original Article, Female, 030211 gastroenterology & hepatology, CLINICAL-PRACTICE GUIDELINES, Cohort study, Adult, Hepatitis B virus, medicine.medical_specialty, DISCONTINUATION, VIRUS-INFECTION, GAMMA-GLUTAMYL-TRANSFERASE, Antiviral Agents, 03 medical and health sciences, Hepatitis B, Chronic, SDG 3 - Good Health and Well-being, Fatal Outcomes from Stopping Nucleoside Analogues in Hepatitis B, Internal medicine, SEROCONVERSION, medicine, Humans, CONSOLIDATION THERAPY, Hepatology, business.industry, medicine.disease, digestive system diseases, Discontinuation, 030104 developmental biology, Withholding Treatment, Human medicine, business
Abstract

Background: Stopping nucleos(t)ide analogues (NA) after hepatitis B e antigen (HBeAg) seroconversion is associated with high relapse rates in Asian patients, but data in Caucasian cohorts are scarce. Clinical course, outcomes and immunological aspects of chronic hepatitis B infections differ substantially between distinct ethnicities. Aim: The aim of this study was to determine relapse rates, factors predicting relapse and clinical outcomes after nucleos(t)ide analogue cessation in a large, predominantly Caucasian cohort of chronic hepatitis B patients with nucleos(t)ide analogue-induced HBeAg seroconversion. Methods: This is a nationwide observational cohort study including HBeAg positive, mono-infected chronic hepatitis B patients with nucleos(t)ide analogue-induced HBeAg seroconversion from 18 centres in Belgium. Results: A total of 98 patients with nucleo(s)tide analogue-induced HBeAg seroconversion were included in the study. Of the 62 patients who stopped treatment after a median consolidation treatment of 8 months, 30 relapsed. Higher gamma-glutamyl transferase levels at both treatment initiation (HR 1.004; P = 0.001 per unit increment) and HBeAg seroconversion (HR 1.006; P = 0.013 per unit increment) were associated with an increased risk of clinically significant relapse in a multivariate Cox regression model. Treatment cessation led to liver-related death in 2 patients, of whom one showed a severe flare. Of the patients who continued treatment after HBeAg seroconversion, none relapsed or developed severe hepatic outcomes. Conclusion: Treatment withdrawal in Caucasian chronic hepatitis B patients after nucleos(t)ide analogue-induced HBeAg seroconversion results in viral relapses in more than half of patients with potential fatal outcomes. These real-world data further lend support to preferentially continue NA treatment after HBeAg seroconversion until HBsAg loss. Foundation Against Cancer Belgium, Grant/Award Number: 2014-087

Published
2018
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18. Enrichment of the tumour immune microenvironment in patients with desmoplastic colorectal liver metastasis

Author

Höppener, D.J. (Diederik J.), Nierop, P.M.H. (Pieter M. H.), Hof, J. (Joost), Sideras, K. (Kostandinos), Zhou, G. (Guoying), Visser, L. (Lydia), Gouw, A.S.H. (Annette), Jong, K.P. (Koert) de, Sprengers, D. (Dave), Kwekkeboom, J. (Jaap), Vermeulen, P.B. (Peter), Grunhagen, D.J. (Dirk Jan), Verhoef, C. (Kees), Höppener, D.J. (Diederik J.), Nierop, P.M.H. (Pieter M. H.), Hof, J. (Joost), Sideras, K. (Kostandinos), Zhou, G. (Guoying), Visser, L. (Lydia), Gouw, A.S.H. (Annette), Jong, K.P. (Koert) de, Sprengers, D. (Dave), Kwekkeboom, J. (Jaap), Vermeulen, P.B. (Peter), Grunhagen, D.J. (Dirk Jan), and Verhoef, C. (Kees)

Abstract

Background: Patients with resected colorectal liver metastasis (CRLM) who display only the desmoplastic histopathological growth pattern (dHGP) exhibit superior survival compared to patients with any non-desmoplastic growth (non-dHGP). The aim of this study was to compare the tumour microenvironment between dHGP and non-dHGP. Methods: The tumour microenvironment was investigated in three cohorts of chemo-naive patients surgically treated for CRLM. In cohort A semi-quantitative immunohistochemistry was performed, in cohort B intrat

Published
2020
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19. LGR5 marks targetable tumor-initiating cells in mouse liver cancer

Author

Cao, W. (Wanlu), Li, M. (Meng), Liu, J. (Jiaye), Zhang, S. (Shaoshi), Noordam, L. (Lisanne), Verstegen, M.M.A. (Monique), Wang, L. (Ling), Ma, B. (Buyun), Li, S. (Shan), Wang, W. (Wenshi), Bolkestein, M. (Michiel), Doukas, M. (Michael), Chen, K. (Kan), Ma, Z. (Zhongren), Bruno, M.J. (Marco), Sprengers, D. (Dave), Kwekkeboom, J. (Jaap), J. W. van der Laan, L. (Luc), Smits, M.J.M. (Ron), Peppelenbosch, M.P. (Maikel), Pan, Q. (Qiuwei), Cao, W. (Wanlu), Li, M. (Meng), Liu, J. (Jiaye), Zhang, S. (Shaoshi), Noordam, L. (Lisanne), Verstegen, M.M.A. (Monique), Wang, L. (Ling), Ma, B. (Buyun), Li, S. (Shan), Wang, W. (Wenshi), Bolkestein, M. (Michiel), Doukas, M. (Michael), Chen, K. (Kan), Ma, Z. (Zhongren), Bruno, M.J. (Marco), Sprengers, D. (Dave), Kwekkeboom, J. (Jaap), J. W. van der Laan, L. (Luc), Smits, M.J.M. (Ron), Peppelenbosch, M.P. (Maikel), and Pan, Q. (Qiuwei)

Abstract

Cancer stem cells (CSCs) or tumor-initiating cells (TICs) are thought to be the main drivers for disease progression and treatment resistance across various cancer types. Identifying and targeting these rare cancer cells, however, remains challenging with respect to therapeutic benefit. Here, we report the enrichment of LGR5 expressing cells, a well-recognized stem cell marker, in mouse liver tumors, and the upregulation of LGR5 expression in human hepatocellular carcinoma. Isolated LGR5 expressing cells from mouse liver tumors are superior in initiating organoids and forming tumors upon engraftment, featuring candidate TICs. These cells are resistant to conventional treatment including sorafenib and 5-FU. Importantly, LGR5 lineage ablation significantly inhibits organoid initiation and tumor growth. The combination of LGR5 ablation with 5-FU, but not sorafenib, further augments the therapeutic efficacy in vivo. Thus, we have identified the LGR5+ compartment as an important TIC population, representing a viable therapeutic target for combating liver cancer.

Published
2020
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25. Immunosuppressive drug withdrawal late after liver transplantation improves the lipid profile and reduces infections

Author

Duizendstra, A. (Aafke), Knegt, R.J. (Robert) de, Betjes, M.G.H. (Michiel), Coenen, S. (Sandra), Darwish Murad, S. (Sarwa), Man, R.A. (Robert) de, Metselaar, H.J. (Herold), Sprengers, D. (Dave), Litjens, N.H.R. (Nicolle), Kwekkeboom, J. (Jaap), Duizendstra, A. (Aafke), Knegt, R.J. (Robert) de, Betjes, M.G.H. (Michiel), Coenen, S. (Sandra), Darwish Murad, S. (Sarwa), Man, R.A. (Robert) de, Metselaar, H.J. (Herold), Sprengers, D. (Dave), Litjens, N.H.R. (Nicolle), and Kwekkeboom, J. (Jaap)

Abstract

BACKGROUND: Treatment with immunosuppressive drugs (IS) after transplantation is accompanied by severe side effects. A limited number of studies have investigated the effect of IS withdrawal on IS-related comorbidities after liver transplantation (LTx) and the results are contradictory. PATIENTS AND METHODS: We determined in a retrospective case-control study the clinical effects of complete IS withdrawal in operationally tolerant (TOL) LTx recipients who discontinued IS 10.8 ± 5.1 years after LTx (n = 13) compared with a completely matched control (CTRL) group with a regular IS regimen (n = 22). TOL recipients have been IS and rejection free for 4.0 ± 2.8 years. RESULTS: IS withdrawal in TOL recipients resulted in lower low-density lipoprotein levels (P = 0.027), whereas this was not observed in the CTRL group. Furthermore, persistent infections in individual recipients were resolved successfully by IS withdrawal. TOL recipients also had significantly fewer de novo infections after IS withdrawal (TOL pre vs. post withdrawal P = 0.0247) compared with recipients continued on IS during the same follow-up period (post withdrawal TOL vs. CTRL P = 0.044). Unfortunately, no improvement in kidney function, and lower rates of de novo occurrences of diabetes, hypertension, cardiovascular diseases, and malignancies were observed in the TOL group after IS withdrawal compared with the CTRL group during the same follow-up time period. CONCLUSION: IS withdrawal late after LTx reduces infection rates and low-density lipoprotein levels, but other IS-related side effects persist late after LTx. An accurate tolerance immune profile enabling identification of tolerant LTx recipients eligible for safe IS withdrawal earlier after transplantation is needed to prevent the development of irreversible IS-related side effects.

Published
2019
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26. Caucasian Ethnicity, but Not Treatment Cessation is Associated with HBsAg Loss Following Nucleos(t)ide Analogue-Induced HBeAg Seroconversion

Author

Hees, S.V. (Stijn Van), Chi, H. (Heng), Hansen, B.E. (Bettina), Bourgeois, S. (Stefan), Vlierberghe, H.V. (Hans Van), Sersté, T. (Thomas), Francque, S. (Sven), Wong, D. (David), Sprengers, D. (Dirk), Moreno, C. (Christophe), Nevens, F. (Frederik), Janssen, H.L.A. (Harry), Vanwolleghem, T. (Thomas), Hees, S.V. (Stijn Van), Chi, H. (Heng), Hansen, B.E. (Bettina), Bourgeois, S. (Stefan), Vlierberghe, H.V. (Hans Van), Sersté, T. (Thomas), Francque, S. (Sven), Wong, D. (David), Sprengers, D. (Dirk), Moreno, C. (Christophe), Nevens, F. (Frederik), Janssen, H.L.A. (Harry), and Vanwolleghem, T. (Thomas)

Abstract

It is well appreciated that ethnicity influences the natural history and immune responses during a chronic hepatitis B infection. In this study, we explore the effect of ethnicity and treatment cessation on Hepatitis B surface Antigen (HBsAg) seroclearance in patients with Nucleos(t)ide Analogue (NA)-induced Hepatitis B e Antigen (HBeAg) seroconversion. We performed a multi-ethnic, multicentric observational cohort study. The analyzed cohort consisted of 178 mono-infected, predominantly male (75.3%) chronic hepatitis B patients of mixed ethnicity (44.4% Asians, 48.9% Caucasians) with nucleos(t)ide analogue-induced HBeAg seroconversion. Treatment was withdrawn in 105 patients and continued in 73, leading to HBsAg loss in 14 patients off- and 16 patients on-treatment, respectively. Overall, HBsAg loss rates were not affected by treatment cessation (hazard ratio 1.45, p = 0.372), regardless of consolidation treatment duration. Caucasian ethnicity was associated with an increased chance of HBsAg loss (hazard ratio 6.70, p = 0.001), but hepatitis B virus genotype was not (p = 0.812). In conclusion, ethnicity is the most important determinant for HBsAg loss after NA-induced HBeAg seroconversion, with up to six-fold higher HBsAg loss rates in Caucasians compared to Asians, irrespective of treatment cessation and consolidation treatment duration.

Published
2019
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27. GITR ligation enhances functionality of tumor-infiltrating T cells in hepatocellular carcinoma

Author

van Beek, A.A., Zhou, GY, Doukas, M., Boor, P.P.C. (Patrick), Noordam, L., Mancham, S. (Shanta), Carrascosa, L.C., van der Heide-Mulder, M, Polak, W.G. (Wojciech), IJzermans, J.N.M. (Jan), Pan, Q. (Qiuwei), Heirman, C. (Carlo), Mahne, A., Bucktrout, S.L., Bruno, M.J. (Marco), Sprengers, D. (Dave), Kwekkeboom, J. (Jaap), van Beek, A.A., Zhou, GY, Doukas, M., Boor, P.P.C. (Patrick), Noordam, L., Mancham, S. (Shanta), Carrascosa, L.C., van der Heide-Mulder, M, Polak, W.G. (Wojciech), IJzermans, J.N.M. (Jan), Pan, Q. (Qiuwei), Heirman, C. (Carlo), Mahne, A., Bucktrout, S.L., Bruno, M.J. (Marco), Sprengers, D. (Dave), and Kwekkeboom, J. (Jaap)

Published
2019
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28. Circulating levels of PD-L1 and Galectin-9 are associated with patient survival in surgically treated Hepatocellular Carcinoma independent of their intra-tumoral expression levels

Author

Sideras, K. (Kostandinos), Man, R.A. (Robert) de, Harrington, S.M. (Susan M.), Polak, W.G. (Wojciech), Zhou, G. (Guoying), Schutz, H.M. (Hannah M.), Pedroza-Gonzalez, A. (Alexander), Biermann, K. (Katharina), Mancham, S. (Shanta), Hansen, B.E. (Bettina), Takkenberg, R.B. (Bart), Vuuren, A.J. (Hanneke) van, Pan, Q. (Qiuwei), IJzermans, J.N.M. (Jan), Sleijfer, S. (Stefan), Sprengers, D. (Dave), Dong, H. (Haidong), Kwekkeboom, J. (Jaap), Bruno, M.J. (Marco), Sideras, K. (Kostandinos), Man, R.A. (Robert) de, Harrington, S.M. (Susan M.), Polak, W.G. (Wojciech), Zhou, G. (Guoying), Schutz, H.M. (Hannah M.), Pedroza-Gonzalez, A. (Alexander), Biermann, K. (Katharina), Mancham, S. (Shanta), Hansen, B.E. (Bettina), Takkenberg, R.B. (Bart), Vuuren, A.J. (Hanneke) van, Pan, Q. (Qiuwei), IJzermans, J.N.M. (Jan), Sleijfer, S. (Stefan), Sprengers, D. (Dave), Dong, H. (Haidong), Kwekkeboom, J. (Jaap), and Bruno, M.J. (Marco)

Abstract

Tumor expression of immune co-inhibitory ligands, such as PD-L1 and Galectin-9, have potential prognostic value in Hepatocellular Carcinoma (HCC). Circulating levels of these molecules, however, have hardly been studied. This study aims to assess the prognostic significance of circulating PD-L1 and circulating Galectin-9 in patients with resected HCC, and to compare their prognostic significance to the intra-tumoral expression of these same molecules. Archived tissues and stored peripheral blood samples from 81 patients who underwent HCC resection or liver transplantation, with curative intent, were used. Immunohistochemistry was performed to determine intra-tumoral expression of PD-L1 and Galectin-9, while ELISA was used to quantify their respective circulating levels. High circulating PD-L1 (HR 0.12, 95%CI 0.16–0.86, p = 0.011) and high circulating Galectin-9 (HR 0.11, 95%CI 0.15–0.85, p = 0.010) levels were both associated with improved HCC-specific survival. Surprisingly, there was no correlation between circulating levels of PD-L1 and Galectin-9 and their intra-tumoral

Published
2019
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29. Caucasian Ethnicity, but Not Treatment Cessation Is Associated with HBsAg Loss Following Nucleos(t)ide Analogue-Induced HBeAg Seroconversion

Author

Hees, Stijn, Chi, Heng, Hansen, Bettina, Bourgeois, S, van Vlierberghe, H, Serste, T, Francque, S, Wong, D, Sprengers, D, Moreno, C, Nevens, F, Janssen, HLA, Vanwolleghem, Thomas, Hees, Stijn, Chi, Heng, Hansen, Bettina, Bourgeois, S, van Vlierberghe, H, Serste, T, Francque, S, Wong, D, Sprengers, D, Moreno, C, Nevens, F, Janssen, HLA, and Vanwolleghem, Thomas

Published
2019

31. Impact of Safety-Related Dose Reductions or Discontinuations on Sustained Virologic Response in HCV-Infected Patients: Results from the GUARD-C Cohort

Author

GUARD C, Study Group, Hassanein, T, Bakalos, G, Ahlers, S, Shiffman, Ml, Tallarico, L, Reddy, Kr, Orlandini, A, Ferenci, P, Derbala, M, Coppola, C, Foster, Gr, Basho, J, Shabanaj, G, Harxhi, A, Debzi, N, Afredj, N, Guessab, N, Mahindad, N, Mahiou, H, Aissaoui, M, Al Qameesh, J, Al Ghandoor, Z, Assene, C, Bastens, B, Brixko, C, Cool, M, De Galocsy, C, Delwaide, J, George, C, Laukens, P, Lefebvre, V, Mulkay, Jp, Nevens, F, Servais, B, Van Vlierberghe, H, Horsmans, Y, Henrion, J, Sprengers, D, Michielsen, P, Bourgeois, S, Lasser, L, Langlet, P, Robaeys, G, Martinet, Jp, Warzee, P, Hoste, P, Reynaert, H, Juriens, I, Decaestecker, J, Van Der Meersch, F, Janssens, F, Ahmetagic, S, Verhaz, A, Bevanda, M, Calkic, L, Ibrahimpasic, N, Mesihovic, R, Mello, Ce, Ruiz, Fj, Martins Junior, E, Ferraz, Ml, Silva, G, Mendes, C, Lyra, A, Silva, Mh, Gomide, G, Fernandes, Jc, Pereira, P, Correa, Mc, Teixeira, R, Yousry, A, Hanno, A, Gabr, M, Omar, A, Esmat, G, Karatapanis, S, Nikolopoulou, V, Giannoulis, G, Manolakopoulos, S, Elefsiniotis, I, Drakoulis, C, Dimitroulopoulos, D, Kanatakis, S, Ketikoglou, I, Mimidis, K, Evgenidis, N, Akriviades, E, Vafiadi Zoubouli, I, Tsianos, E, Mela, M, Orfanou, E, Mousoulis, G, Karagiannis, I, Manesis, E, Varga, M, Nemesánszky, E, Fried, K, Schuller, J, Szalay, F, Lengyel, G, Tornai, I, Banyai, T, Lesch, M, Nagy, I, Gervain, J, Tusnadi, A, Schneider, F, Szentgyörgyi, L, Hunyady, B, Vincze, A, Tolvaj, G, Varkonyi, I, Makkai, E, Enyedi, J, Racz, I, Hausinger, P, Váczi, Z, Patai, Á, Ozsvár, Z, Lakner, L, Ribiczey, P, Bhalla, A, Somani, S, Luaia, R, Rao, P, Philip, M, Lawate, P, Nagral, A, Sood, A, Parikh, S, Merat, S, Nassiri Toosi, M, Alavian, Sm, Zali, Mr, Daryani, Ne, Drenaggi, D, Attili, Af, Bandiera, F, Bassi, P, Bellati, G, Bellantani, S, Brunetto, MAURIZIA ROSSANA, Bruno, S, Castelli, F, Castellacci, R, Cattelan, Am, Colombo, M, Craxi, A, D'Angelo, S, Colombo, S, Demelia, L, Di Perri, G, Di Giacomo, A, Ferrari, C, Francisci, D, Casinelli, K, Ganga, R, Costa, C, Mangia, A, Russo, Fp, Matarazzo, F, Mazzella, G, Mazzeo, M, Memoli, M, Montalbano, M, Montalto, G, Pieri, A, Passariello, N, Picciotto, A, Pietrangelo, A, Pirisi, M, Quirino, T, Raimondo, G, Rapaccini, Gl, Rizzardini, G, Rizzetto, M, Russello, M, Sabusco, G, Santantonio, T, Soardo, G, Amedea, A, Verucchi, G, Vinelli, F, Zignego, Al, Zuin, M, Ascione, A, Vinci, M, Pigozzi, Mg, Tundo, P, Saracco, Gm, Amoroso, P, Andreoni, M, Colletta, C, Erne, E, Megna, As, Biglino, A, Chiriaco, P, Foti, G, Spinzi, G, D'Amico, E, Paik, Sw, Ahn, Sh, Lee, Yn, Kim, Y, Yang, J, Han, Sy, Varghese, R, Al Gharabally, A, Askar, H, Sharara, A, Yaghi, C, Rached, Aa, Houmani, Z, Zaarour, F, Dohaibi, A, Ivanovski, L, Joksimovic, N, Abbas, Z, Memon, S, Mohsin, A, Masood, S, Hashmi, Z, Halota, W, Deron, Z, Mazur, W, Flisiak, R, Lipczynski, A, Musialik, J, Piekarska, A, Augustyniak, K, Baka Cwierz, B, Simon, K, Gietka, A, Berak, H, Sieklucki, J, Radowska, D, Szlauer, B, Piekos, T, Olszok, I, Jablkowski, M, Orszulak, G, Warakomska, I, Aleixo, Mj, Valente, C, Macedo, G, Sarmento Castro, R, Roxo, F, Faria, T, Mansinho, K, Velez, J, Ramos, Jp, Guerreiro, H, Alberto, S, Monteverde, C, Serejo, F, Peixe, P, Malhado, J, Curescu, M, Streinu Cercel, A, Caruntu, F, Livia, H, Preotescu, L, Arama, V, Ancuta, I, Gheorghe, L, Stanciu, C, Trifan, A, Acalovschi, M, Andreica, V, Pascu, O, Lencu, M, Sporea, I, Olteanu, D, Ionita Radu, F, Fierbinteanu Braticevici, C, Motoc, A, Silaghi, R, Musat, M, Coman, F, Stan, M, Cijevschi, C, Miftode, E, Delic, D, Jesic, R, Nozic, D, Svorcan, P, Fabri, M, Konstantinovic, L, Pelemis, M, Jankovic, G, Todorovic, Z, Nagorni, A, Kupcova, V, Skladany, L, Szantova, M, Krkoska, D, Jarcuska, P, Schreter, I, Oltman, M, Bocakova, J, Bunganic, I, Holoman, J, Giguere, A, Abdou, A. M., Basic (bio-) Medical Sciences, Gastroenterology, Laboratory of Molecullar and Cellular Therapy, Liver Cell Biology, Michielsen, Peter, GUARD-C Study Group, Graham R. Foster, Carmine Coppola, Moutaz Derbala, Peter Ferenci, Alessandra Orlandini, K. Rajender Reddy, Ludovico Tallarico, Mitchell L. Shiffman, Silke Ahler, Georgios Bakalo, Tarek Hassanein, GUARD-C Study Group: [.., Davide Drenaggi, Adolfo Francesco Attili, Franco Bandiera, Paolo Bassi, Giorgio Bellati, Stefano Bellantani, Maurizia Brunetto, Savino Bruno, Francesco Castelli, Roberto Castellacci, Anna Maria Cattelan, Massimo Colombo, Antonio Craxi, Salvatore D'angelo, Silvia Colombo, Luigi Demelia, Giovanni Di Perri, Antonio Di Giacomo, Carlo Ferrari, Daniela Francisci, Katia Casinelli, Roberto Ganga, Chiara Costa, Alessandra Mangia, Francesco Paolo Russo, Filippo Matarazzo, Giuseppe Mazzella, Maurizio Mazzeo, Massimo Memoli, Marzia Montalbano, Giuseppe Montalto, Alessandro Pieri, Nicola Passariello, Antonio Picciotto, Antonello Pietrangelo, Mario Pirisi, Tiziana Quirino, Giovanni Raimondo, Gian Ludovico Rapaccini, Giuliano Rizzardini, Mario Rizzetto, Maurizio Russello, Giuseppe Sabusco, Teresa Santantonio, Giorgio Soardo, Alessandri Amedea, Gabriella Verucchi, Francesco Vinelli, Anna Linda Zignego, Massimo Zuin, Antonio Ascione, Maria Vinci, Maria Graziella Pigozzi, Paolo Tundo, Giorgio Maria Saracco, Pietro Amoroso, Massimo Andreoni, Cosimo Colletta, Elke Erne, Angelo Salomone Megna, Alberto Biglino, Piergiorgio Chiriaco, Giuseppe Foti, Giancarlo Spinzi, Emilio D'amico, …], Foster G.R., Coppola C., Derbala M., Ferenci P., Orlandini A., Reddy K.R., Tallarico L., Shiffman M.L., Ahlers S., Bakalos G., Hassanein T., Basho J., Shabanaj G., Harxhi A., Debzi N., Afredj N., Guessab N., Mahindad N., Mahiou H., Aissaoui M., Al Qameesh J., Al Ghandoor Z., Assene C., Bastens B., Brixko C., Cool M., De Galocsy C., Delwaide J., George C., Laukens P., Lefebvre V., Mulkay J.-P., Nevens F., Servais B., Van Vlierberghe H., Horsmans Y., Henrion J., Sprengers D., Michielsen P., Bourgeois S., Lasser L., Langlet P., Robaeys G., Martinet J.-P., Warzee P., Hoste P., Reynaert H., Juriens I., Decaestecker J., Van Der Meersch F., Janssens F., Ahmetagic S., Verhaz A., Bevanda M., Calkic L., Ibrahimpasic N., Mesihovic R., Mello C.E., Ruiz F.J., Junior E.M., Ferraz M.L., Silva G., Mendes C., Lyra A., Silva M.H., Gomide G., Fernandes J.C., Pereira P., Correa M.C., Teixeira R., Yousry A., Hanno A., Gabr M., Omar A., Esmat G., Karatapanis S., Nikolopoulou V., Giannoulis G., Manolakopoulos S., Elefsiniotis I., Drakoulis C., Dimitroulopoulos D., Kanatakis S., Ketikoglou I., Mimidis K., Evgenidis N., Akriviades E., Vafiadi-Zoubouli I., Tsianos E., Mela M., Orfanou E., Mousoulis G., Karagiannis I., Manesis E., Varga M., Nemesanszky E., Fried K., Schuller J., Szalay F., Lengyel G., Tornai I., Banyai T., Lesch M., Nagy I., Gervain J., Tusnadi A., Schneider F., Szentgyorgyi L., Hunyady B., Vincze A., Tolvaj G., Varkonyi I., Makkai E., Enyedi J., Racz I., Hausinger P., Vaczi Z., Patai A., Ozsvar Z., Lakner L., Ribiczey P., Bhalla A., Somani S., Luaia R., Rao P., Philip M., Lawate P., Nagral A., Sood A., Parikh S., Merat S., Nassiri-Toosi M., Alavian S.-M., Zali M.R., Daryani N.E., Drenaggi D., Attili A.F., Bandiera F., Bassi P., Bellati G., Bellantani S., Brunetto M., Bruno S., Castelli F., Castellacci R., Cattelan A.M., Colombo M., Craxi A., D'angelo S., Colombo S., Demelia L., Di Perri G., Di Giacomo A., Ferrari C., Francisci D., Casinelli K., Ganga R., Costa C., Mangia A., Russo F.P., Matarazzo F., Mazzella G., Mazzeo M., Memoli M., Montalbano M., Montalto G., Pieri A., Passariello N., Picciotto A., Pietrangelo A., Pirisi M., Quirino T., Raimondo G., Rapaccini G.L., Rizzardini G., Rizzetto M., Russello M., Sabusco G., Santantonio T., Soardo G., Amedea A., Verucchi G., Vinelli F., Zignego A.L., Zuin M., Ascione A., Vinci M., Pigozzi M.G., Tundo P., Saracco G.M., Amoroso P., Andreoni M., Colletta C., Erne E., Megna A.S., Biglino A., Chiriaco P., Foti G., Spinzi G., D'amico E., Paik S.W., Ahn S.-H., Lee Y.N., Kim Y., Yang J., Han S.Y., Varghese R., Al Gharabally A., Askar H., Sharara A., Yaghi C., Abou Rached A., Houmani Z., Zaarour F., Dohaibi A., Ivanovski L., Joksimovic N., Abbas Z., Memon S., Mohsin A., Masood S., Hashmi Z., Halota W., Deron Z., Mazur W., Flisiak R., Lipczynski A., Musialik J., Piekarska A., Augustyniak K., Baka-Cwierz B., Simon K., Gietka A., Berak H., Sieklucki J., Radowska D., Szlauer B., Piekos T., Olszok I., Jablkowski M., Orszulak G., Warakomska I., Aleixo M.J., Valente C., Macedo G., Sarmento-Castro R., Roxo F., Faria T., Mansinho K., Velez J., Ramos J.P., Guerreiro H., Alberto S., Monteverde C., Serejo F., Peixe P., Malhado J., Curescu M., Streinu-Cercel A., Caruntu F., Livia H., Preotescu L., Arama V., Ancuta I., Gheorghe L., Stanciu C., Trifan A., Acalovschi M., Andreica V., Pascu O., Lencu M., Sporea I., Olteanu D., Ionita-Radu F., Fierbinteanu-Braticevici C., Motoc A., Silaghi R., Musat M., Coman F., Stan M., Cijevschi C., Miftode E., Delic D., Jesic R., Nozic D., Svorcan P., Fabri M., Konstantinovic L., Pelemis M., Jankovic G., Todorovic Z., Nagorni A., Kupcova V., Skladany L., Szantova M., Krkoska D., Jarcuska P., Schreter I., Oltman M., Bocakova J., Bunganic I., Holoman J., Giguere A., Abdou A.M.S., UCL - SSS/IREC-Institut de recherche expérimentale et clinique, UCL - SSS/IREC/GAEN-Pôle d'Hépato-gastro-entérologie, and UCL - (SLuc) Service de gastro-entérologie

Subjects
Genetics and Molecular Biology (all), Male, Chronic Hepatitis, Hepacivirus, Ribavirin/adverse effects, Asthenia/chemically induced, Polyethylene Glycol, Biochemistry, Polyethylene Glycols, Body Mass Index, Chronic Liver Disease, 0302 clinical medicine, Neutropenia/chemically induced, Interferon-alpha/adverse effects, Medicine, Chronic, lcsh:Science, Liver Diseases, virus diseases, Antiviral Agents/adverse effects, Cohort, Science & Technology - Other Topics, 030211 gastroenterology & hepatology, Drug Therapy, Combination, Cohort study, Human, medicine.medical_specialty, Alpha interferon, Gastroenterology and Hepatology, Antiviral Agents, Microbiology, Dose-Response Relationship, 03 medical and health sciences, Pharmacotherapy, Hepatitis C, Chronic/drug therapy, Dose Prediction Methods, Drug Therapy, Anemia/chemically induced, Humans, Hemoglobin, Aged, Medicine and health sciences, Biochemistry, Genetics and Molecular Biology (all), Hepaciviru, Science & Technology, Dose-Response Relationship, Drug, Flaviviruses, lcsh:R, Organisms, Biology and Life Sciences, Proteins, medicine.disease, digestive system diseases, chemistry, Agricultural and Biological Sciences (all), Withholding Treatment, Asthenia, Immunology, Proportional Hazards Model, lcsh:Q, Human medicine, RNA viruses, Physiology, lcsh:Medicine, Peginterferon-alfa, Polyethylene Glycols/adverse effects, Adult, Anemia, Cohort Studies, Female, Hepatitis C, Chronic, Host-Pathogen Interactions, Interferon-alpha, Middle Aged, Neutropenia, Outcome Assessment (Health Care), Proportional Hazards Models, RNA, Viral, Recombinant Proteins, Ribavirin, Medicine (all), chemistry.chemical_compound, Outcome Assessment, Health Care, Medicine and Health Sciences, 030212 general & internal medicine, Viral, Pathology and laboratory medicine, Multidisciplinary, biology, Hepatitis C virus, Pharmaceutics, Hepatitis C, Hematology, Recombinant Protein, Outcome Assessment (Health Care)/methods, Medical microbiology, Host-Pathogen Interaction, Multidisciplinary Sciences, Physiological Parameters, Research Design, Combination, Viruses, Drug, Pathogens, Host-Pathogen Interactions/drug effects, Research Article, Clinical Research Design, Research and Analysis Methods, Internal medicine, Recombinant Proteins/adverse effects, RNA, Viral/blood, Antiviral Agent, business.industry, Body Weight, Hepacivirus/drug effects, Viral pathogens, biology.organism_classification, Hepatitis viruses, Microbial pathogens, RNA, Adverse Events, Cohort Studie, business
Abstract

Background: Despite the introduction of direct-acting antiviral agents for chronic hepatitis C virus (HCV) infection, peginterferon alfa/ribavirin remains relevant in many resource-constrained settings. The non-randomized GUARD-C cohort investigated baseline predictors of safety-related dose reductions or discontinuations (sr-RD) and their impact on sustained virologic response (SVR) in patients receiving peginterferon alfa/ribavirin in routine practice. Methods: A total of 3181 HCV-mono-infected treatment-naive patients were assigned to 24 or 48 weeks of peginterferon alfa/ribavirin by their physician. Patients were categorized by time-to-first sr-RD (Week 4/12). Detailed analyses of the impact of sr-RD on SVR24 (HCV RNA

Published
2015

32. Prognostic value of intra-tumoral CD8+/FoxP3+ lymphocyte ratio in patients with resected colorectal cancer liver metastasis

Author

Sideras, K. (Kostandinos), Galjart, B. (Boris), Vasaturo, A. (Angela), Pedroza-Gonzalez, A. (Alexander), Biermann, K. (Katharina), Mancham, S. (Shanta), Nigg, A.L. (Alex), Hansen, B.E. (Bettina), Stoop, H.A. (Hans A.), Zhou, G. (Guoying), Verhoef, C. (Kees), Sleijfer, S. (Stefan), Sprengers, D. (Dave), Kwekkeboom, J. (Jaap), Bruno, M.J. (Marco), Sideras, K. (Kostandinos), Galjart, B. (Boris), Vasaturo, A. (Angela), Pedroza-Gonzalez, A. (Alexander), Biermann, K. (Katharina), Mancham, S. (Shanta), Nigg, A.L. (Alex), Hansen, B.E. (Bettina), Stoop, H.A. (Hans A.), Zhou, G. (Guoying), Verhoef, C. (Kees), Sleijfer, S. (Stefan), Sprengers, D. (Dave), Kwekkeboom, J. (Jaap), and Bruno, M.J. (Marco)

Abstract

Background and Objectives: Patients with isolated colorectal-cancer-liver-metastases (CRCLM) frequently undergo metastatectomy. Tumor-infiltrating-lymphocytes (TILs) have prognostic potential in the setting of primary colorectal cancer, however, their role in CRCLM is less studied. We aimed to study the spatial distribution and prognostic role of tumor-infiltrating CD8+ cytotoxic T-cells and FoxP3+ regulatory T-cells at the metastatic site of CRCLM patients. Methods: TILs were isolated from fresh metastatic tissues of 47 patients with CRCLM. Archived paraffin-embedded tissue, from the same patients, was retrieved. CD8+ and FoxP3+ cells, both in the intra-tumoral and the peri-tumoral compartments, were measured by immunohistochemistry on full tissue sections. Proportions of cytotoxic T-cells (CD8+) and regulatory T-cells (CD4+CD25+FoxP3+), within CD45+TILs, were measured by flow-cytometry. Results: By immunohistochemistry, individual densities of intra-tumoral or peri-tumoral CD8+ and FoxP3+ cells were not prognostic of survival. However, the intra-tumoral, but not the peri-tumoral, CD8+/FoxP3+ ratio was an independent predictor of survival (HR 0.43, 95%CI 0.19-0.95, P = 0.032). By flow cytometry, the intra

Published
2018
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33. Protocol for the STRONG trial: stereotactic body radiation therapy following chemotherapy for unresectable perihilar cholangiocarcinoma, a phase I feasibility study

Author

Koedijk, M.S. (Merel S.), Heijmen, B.J.M. (Ben), Groot Koerkamp, B. (Bas), Eskens, F.A.L.M. (Ferry), Sprengers, D. (Dave), Poley, J.-W. (Jan-Werner), van Gent, D.C. (Dik C.), Laan, L.J.W. (Luc) van der, Holt, B. (Bronno) van der, Willemssen, F.E.J.A. (François), Méndez Romero, A.M. (Alejandra), Koedijk, M.S. (Merel S.), Heijmen, B.J.M. (Ben), Groot Koerkamp, B. (Bas), Eskens, F.A.L.M. (Ferry), Sprengers, D. (Dave), Poley, J.-W. (Jan-Werner), van Gent, D.C. (Dik C.), Laan, L.J.W. (Luc) van der, Holt, B. (Bronno) van der, Willemssen, F.E.J.A. (François), and Méndez Romero, A.M. (Alejandra)

Abstract

INTRODUCTION: For patients with perihilar cholangiocarcinoma (CCA), surgery is the only treatment modality that can result in cure. Unfortunately, in the majority of these patients, the tumours are found to be unresectable at presentation due to either local invasive tumour growth or the presence of distant metastases. For patients with unresectable CCA, palliative chemotherapy is the standard treatment yielding an estimated median overall survival (OS) of 12-15.2 months. There is no evidence from randomised trials to support the use of stereotactic body radiation therapy (SBRT) for CCA. However, small and most often retrospective studies combining chemotherapy with SBRT have shown promising results with OS reaching up to 33-35 months.METHODS AND ANALYSIS: This study has been designed as a single-centre phase I feasibility trial and will investigate the addition of SBRT after standard chemotherapy in patients with unresectable perihilar CCA (T1-4 N0-1 M0). A total of six patients will be included. SBRT will be delivered in 15 fractions of 3-4.5 Gy (risk adapted). The primary objective of this study is to determine feasibility and toxicity. Secondary outcomes include local tumour control, progression-free survival (PFS), OS and quality of life. Length of follow-up will be 2 years. As an ancillary study, the personalised effects of radiotherapy will be measured in vitro, in patient-derived tumour and bile duct organoid cultures.ETHICS AND DISSEMINATION: Ethics approval for the STRONG trial has been granted by the Medical Ethics Committee of Erasmus MC Rotterdam, the Netherlands. It is estimated that all patients will be included between October 2017 and October 2018. The results of this study will be published in a peer-reviewed journal, and presented at national and international conferences.TRIAL REGISTRATION NUMBER: NCT03307538; Pre-results.

Published
2018
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34. Blockade of LAG3 enhances responses of tumor-infiltrating T cells in mismatch repair-proficient liver meta

Author

Zhou, G. (Guoying), Noordam, L. (Lisanne), Sprengers, D. (Dave), Doukas, M. (Michail), Boor, P.P.C. (Patrick), Beek, A.A. (Adriaan) van, Erkens, R. (Remco), Mancham, S. (Shanta), Grunhagen, D.J. (Dirk Jan), Menon, A.G. (Anand), Lange, J.F. (Johan), Burger, P.J.W.A. (Pim J. W. A.), Brandt, A. (Alexandra), Galjart, B. (Boris), Verhoef, C. (Kees), Kwekkeboom, J. (Jaap), Bruno, M.J. (Marco), Zhou, G. (Guoying), Noordam, L. (Lisanne), Sprengers, D. (Dave), Doukas, M. (Michail), Boor, P.P.C. (Patrick), Beek, A.A. (Adriaan) van, Erkens, R. (Remco), Mancham, S. (Shanta), Grunhagen, D.J. (Dirk Jan), Menon, A.G. (Anand), Lange, J.F. (Johan), Burger, P.J.W.A. (Pim J. W. A.), Brandt, A. (Alexandra), Galjart, B. (Boris), Verhoef, C. (Kees), Kwekkeboom, J. (Jaap), and Bruno, M.J. (Marco)

Abstract

Purpose: Liver metastasis develops in >50% of patients with colorectal cancer (CRC), and is a leading cause of CRC-related mortality. We aimed to identify which inhibitory immune checkpoint pathways can be targeted to enhance functionality of intra-tumoral T-cells in mismatch repair-proficient liver metastases of colorectal cancer (LM-CRC). Methodology: Intra-tumoral expression of multiple inhibitory molecules was compared among mismatch repair-proficient LM-CRC, peritoneal metastases of colorectal cancer (PM-CRC) and primary CRC. Expression of inhibitory molecules was also analyzed on leukocytes isolated from paired resected metastatic liver tumors, tumor-free liver tissues, and blood of patients with mismatch repair-proficient LM-CRC. The effects of blocking inhibitory pathways on tumor-infiltrating T-cell responses were studied in ex vivo functional assays. Results: Mismatch repair-proficient LM-CRC showed higher expression of inhibitory receptors on intra-tumoral T-cells and contained higher proportions of CD8+ T-cells, dendritic cells and monocytes than mismatch repair-proficient primary CRC and/or PM-CRC. Inhibitory receptors LAG3, PD-1, TIM3 and CTLA4 were higher expressed on CD8+ T-cells, CD4+ T-helper and/or regulatory T-cells in LM-CRC tumors compared with tumor-free liver and blood. Antibody blockade of LAG3 or PD-L1 increased proliferation and effector cytokine production of intra-tumoral T-cells isolated from LM-CRC in response to both polyclonal and autologous tumor-specific stimulations. Higher LAG3 expression on intra-tumoral CD8+ T-cells associated with longer progression-free survival of LM-CRC patients. Conclusion: Mismatch repair-proficient LM-CRC may be more sensitive to immune checkpoint inhibitors than mismatch repair-proficient primary CRC. Blocking LAG3 enhances tumor-infiltrating T-cell responses of mismatch repair-proficient LM-CRC, and therefore may be a new promising immunotherapeutic target for LM-CRC.

Published
2018
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36. PD-L1, Galectin-9 and CD8+ tumor-infiltrating lymphocytes are associated with survival in hepatocellular carcinoma

Author

Sideras, K. (Kostandinos), Biermann, K. (Katharina), Verheij, J. (Joanne), Takkenberg, B.R. (Bart R.), Mancham, S. (Shanta), Hansen, B.E. (Bettina), Schutz, H.M. (Hannah M.), Man, R.A. (Robert) de, Sprengers, D. (Dave), Buschow, S.I. (Sonja I.), Verseput, M.C.M. (Maddy C. M.), Boor, P.P.C. (Patrick), Pan, Q. (Qiuwei), Gulik, T.M. (Thomas) van, Terkivatan, T. (Türkan), IJzermans, J.N.M. (Jan), Beuers, U. (Ulrich), Sleijfer, S. (Stefan), Bruno, M.J. (Marco), Kwekkeboom, J. (Jaap), Sideras, K. (Kostandinos), Biermann, K. (Katharina), Verheij, J. (Joanne), Takkenberg, B.R. (Bart R.), Mancham, S. (Shanta), Hansen, B.E. (Bettina), Schutz, H.M. (Hannah M.), Man, R.A. (Robert) de, Sprengers, D. (Dave), Buschow, S.I. (Sonja I.), Verseput, M.C.M. (Maddy C. M.), Boor, P.P.C. (Patrick), Pan, Q. (Qiuwei), Gulik, T.M. (Thomas) van, Terkivatan, T. (Türkan), IJzermans, J.N.M. (Jan), Beuers, U. (Ulrich), Sleijfer, S. (Stefan), Bruno, M.J. (Marco), and Kwekkeboom, J. (Jaap)

Abstract

Novel systemic treatments for hepatocellular carcinoma (HCC) are strongly needed. Immunotherapy is a promising strategy that can induce specific antitumor immune responses. Understanding the mechanisms of immune resistance by HCC is crucial for development of suitable immunotherapeutics. We used immunohistochemistry on tissue-microarrays to examine the co-expression of the immune inhibiting molecules PD-L1, Galectin-9, HVEM and IDO, as well as tumor CD8+ lymphocyte infiltration in HCC, in two independent cohorts of patients. We found that at least some expression in tumor cells was seen in 97% of cases for HVEM, 83% for PD-L1, 79% for Gal-9 and 66% for IDO. In the discovery cohort (n = 94), we found that lack of, or low, tumor expression of PD-L1 (p < 0.001), Galectin-9 (p < 0.001) and HVEM (p < 0.001), and low CD8+TIL count (p = 0.016), were associated with poor HCC-specific survival. PD-L1, Galectin-9 and CD8+TIL count were predictive of HCC-specific survival independent of baseline clinicopathologic characteristics and the combination of these markers was a powerful predictor of HCC-specific survival (HR 0.29; p <0.001). These results were confirmed in the validation cohort (n = 60). We show that low expression levels of PD-L1 and Gal-9 in combination with low CD8+TIL count predict extremely poor HCC-specific survival and it requires a change in two of these parameters to significantly improve prognosis. In conclusion, intra-tumoral expression of these immune inhibiting molecules was observed in the majority of HCC patients. Low expression of PD-L1 and Galectin-9 and low CD8+TIL count are associated with poor HCC-specific survival. Combining immune biomarkers leads to superior predictors of HCC mortality.

Published
2017
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37. Factors associated with ethnical disparity in overall survival for patients with hepatocellular carcinoma

Author

Li, J. (Juan), Hansen, B.E. (Bettina), Peppelenbosch, M.P. (Maikel), Man, R.A. (Robert) de, Pan, Q. (Qiuwei), Sprengers, D. (Dave), Li, J. (Juan), Hansen, B.E. (Bettina), Peppelenbosch, M.P. (Maikel), Man, R.A. (Robert) de, Pan, Q. (Qiuwei), and Sprengers, D. (Dave)

Abstract

Hepatocellular carcinoma (HCC) is an important cause of cancer-related death worldwide. Ethnical disparity in overall survival has been demonstrated for HCC patients in the United States (U.S.). We aimed to evaluate the contributors to this survival disparity. The SEER database was used to identify HCC patients from 2004 to 2012. Kaplan-Meier curves and Cox proportional hazard models were used to evaluate overall survival by ethnicity and the contributors to ethnical survival disparity. A total of 33 062 patients were included: 15 986 Non-Hispanic Whites, 6535 Hispanic Whites, 4842 African Americans, and 5699 Asians. Compared to Non-Hispanic Whites, African Americans had worse survival (HR, 1.18; 95%CI, 1.14-1.23), while Asians had a better survival (HR, 0.85; 95%CI, 0.82-0.89), and Hispanic Whites had a similar survival (HR, 1.01; 95%CI, 0.97-1.05). Multivariate Cox analysis identified that tumor presentation- and treatment-related factors significantly contributed to the ethnical survival disparity. Especially, tumor size was the most important contributor (HR, 1.11; 95%CI, 1.07-1.16). There is no ethnical survival disparity in patients undergoing liver transplantation and sub-analysis of patients within the Milan criteria for liver transplantation demonstrated no significant survival disparity between African Americans and non-Hispanic Whites in transplantation adjustment analysis (HR, 1.23; 95%CI, 1.11-1.35 in non-adjustment analysis to HR, 1.05; 95%CI, 0.95-1.15 after adjustment). Finally, no important contributor to the superior overall survival in Asians was identified. In conclusion, poor tumor presentation at diagnosis, limited benefit from resection and restricted utilization of liver transplantation are important contributors to poorer survival of African Americans with HCC.

Published
2017
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38. Hepatic LGR5 stem cells contribute to liver carcinogenesis

Author

Cao, W., Li, M., Liu, P., Liu, J., Bolkestein, M., Chen, K., Van Der Laan, L. J. W., Sprengers, D., Metselaar, H. J., Kwekkeboom, J., Smits, R., Peppelenbosch, M. P., Pan, Q., Cao, W., Li, M., Liu, P., Liu, J., Bolkestein, M., Chen, K., Van Der Laan, L. J. W., Sprengers, D., Metselaar, H. J., Kwekkeboom, J., Smits, R., Peppelenbosch, M. P., and Pan, Q.

Published
2017

43. Hepatic LGR5 stem cells contribute to liver carcinogenesis

Author

Cao, W., primary, Li, M., additional, Liu, P., additional, Liu, J., additional, Bolkestein, M., additional, Chen, K., additional, Van Der Laan, L.J.W., additional, Sprengers, D., additional, Metselaar, H.J., additional, Kwekkeboom, J., additional, Smits, R., additional, Peppelenbosch, M.P., additional, and Pan, Q., additional

Published
2017
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44. Rapid hepatic clearance of full length CCN-2/CTGF: a putative role for LRP1-mediated endocytosis

Author

Gerritsen, K. G F, Bovenschen, N., Nguyen, T. Q., Sprengers, D., Koeners, M. P., van Koppen, A. N., Joles, J. A., Goldschmeding, R., Kok, R. J., Gerritsen, K. G F, Bovenschen, N., Nguyen, T. Q., Sprengers, D., Koeners, M. P., van Koppen, A. N., Joles, J. A., Goldschmeding, R., and Kok, R. J.

Abstract

CCN-2 (connective tissue growth factor; CTGF) is a key factor in fibrosis. Plasma CCN-2 has biomarker potential in numerous fibrotic disorders, but it is unknown which pathophysiological factors determine plasma CCN-2 levels. The proteolytic amino-terminal fragment of CCN-2 is primarily eliminated by the kidney. Here, we investigated elimination and distribution profiles of full length CCN-2 by intravenous administration of recombinant CCN-2 to rodents. After bolus injection in mice, we observed a large initial distribution volume (454 mL/kg) and a fast initial clearance (120 mL/kg/min). Immunosorbent assay and immunostaining showed that CCN-2 distributed mainly to the liver and was taken up by hepatocytes. Steady state clearance in rats, determined by continuous infusion of CCN-2, was fast (45 mL/kg/min). Renal CCN-2 clearance, determined by arterial and renal vein sampling, accounted for only 12 % of total clearance. Co-infusion of CCN-2 with receptor-associated protein (RAP), an antagonist of LDL-receptor family proteins, showed that RAP prolonged CCN-2 half-life and completely prevented CCN-2 internalization by hepatocytes. This suggests that hepatic uptake of CCN-2 is mediated by a RAP-sensitive mechanism most likely involving LRP1, a member of the LDL-receptor family involved in hepatic clearance of various plasma proteins. Surface plasmon resonance binding studies confirmed that CCN-2 is an LRP1 ligand. Co-infusion of CCN-2 with an excess of the heparan sulphate-binding protamine lowered the large initial distribution volume of CCN-2 by 88 % and reduced interstitial staining of CCN-2, suggesting binding of CCN-2 to heparan sulphate proteoglycans (HSPGs). Protamine did not affect clearance rate, indicating that RAP-sensitive clearance of CCN-2 is HSPG independent. In conclusion, unlike its amino-terminal fragment which is cleared by the kidney, full length CCN-2 is primarily eliminated by the liver via a fast RAP-sensitive, probably LRP1-dependent pathway.

Published
2016

45. Hepatocellular carcinoma in cirrhotic versus noncirrhotic livers: results from a large cohort in the Netherlands

Author

Meer, S de, Erpecum, K.J. van, Sprengers, D., Coenraad, M.J., Klumpen, H.J., Jansen, P.L., JN, I.J., Verheij, J., Nieuwkerk, C.M. van, Siersema, P.D., Man, R.A. de, Meer, S de, Erpecum, K.J. van, Sprengers, D., Coenraad, M.J., Klumpen, H.J., Jansen, P.L., JN, I.J., Verheij, J., Nieuwkerk, C.M. van, Siersema, P.D., and Man, R.A. de

Abstract

Item does not contain fulltext, OBJECTIVES: Hepatocellular carcinoma (HCC) usually occurs in patients with cirrhosis, but can also develop in noncirrhotic livers. In the present study we explored associated risk factors for HCC without cirrhosis and compared patient and tumor characteristics and outcomes in HCC patients with and without underlying cirrhosis. METHODS: Patients with HCC diagnosed in the period 2005-2012 in five Dutch academic centers were evaluated. Patients were categorized according to the presence of cirrhosis on the basis of histology or combined radiological and laboratory features. RESULTS: In total, 19% of the 1221 HCC patients had no underlying cirrhosis. Noncirrhotic HCC patients were more likely to be female and to have nonalcoholic fatty liver disease or no risk factors for underlying liver disease, and less likely to have hepatitis C virus or alcohol-related liver disease than did cirrhotic HCC patients. HCCs in noncirrhotic livers were more often unifocal (67 vs. 48%), but tumor size was significantly larger (8 vs. 4 cm). Despite the larger tumors, more patients underwent resection (50 vs. 10%) and overall survival was significantly better than in cirrhotics. In multivariate analyses, absence of cirrhosis [hazard ratio (HR) 0.49, 95% confidence interval (CI) 0.38-0.63] and presence of hepatitis B (HR 0.68, 95% CI 0.51-0.91) were independent predictors for lower mortality, whereas hepatitis C virus was associated with higher mortality (HR 1.32, 95% CI 1.01-1.65). CONCLUSION: HCC without cirrhosis was strongly associated with female sex and presence of nonalcoholic fatty liver disease or no risk factors for underlying liver disease. In absence of cirrhosis, resections were more often performed, with better survival despite larger tumor size.

Published
2016

46. Hepatocellular carcinoma in noncirrhotic livers is associated with steatosis rather than steatohepatitis: potential implications for pathogenesis

Author

Meer, S. van, Erpecum, K.J. van, Sprengers, D., Klumpen, H.J., Jansen, P.L., Ijzermans, J.N., Siersema, P.D., Man, R.A. de, Verheij, J., Meer, S. van, Erpecum, K.J. van, Sprengers, D., Klumpen, H.J., Jansen, P.L., Ijzermans, J.N., Siersema, P.D., Man, R.A. de, and Verheij, J.

Abstract

Item does not contain fulltext, OBJECTIVE: The risk of hepatocellular carcinoma (HCC) is increased in patients with metabolic syndrome (MS), possibly related to nonalcoholic fatty liver disease (NAFLD). As histological features of NAFLD may regress in cirrhosis, we compared steatosis versus steatohepatitis in the nontumoral liver of noncirrhotic HCC patients. PATIENTS AND METHODS: A retrospective clinicopathological analysis was carried out in 91 noncirrhotic HCC patients. Patients were divided into three subgroups: that is, patients with: (1) MS without other risk factors for underlying liver disease, (2) no underlying risk factors, or (3) other risk factors (with or without MS). The NAFLD activity score (NAS) less than 3 was classified as no steatohepatitis, NAS 3-4 as borderline steatohepatitis, and NAS 5 or more as definite steatohepatitis. RESULTS: Eleven (12%) patients had MS without other risk factors (group 1). In the nontumoral liver, significant steatosis (>/=5% of hepatocytes) was generally present (in 10/11 patients), with mild lobular inflammation and absence of ballooning in most cases. Absence of steatohepatitis, borderline steatohepatitis, and definite steatohepatitis were found in 55, 45, and 0% of cases, respectively. In groups 2 and 3, significant steatosis was frequently present (in 16/37 and 21/43 patients, respectively). Absence of steatohepatitis, borderline steatohepatitis, and definite steatohepatitis were found in 84, 16, and 0% of cases (group 2), respectively, in 77, 23, and 0% of cases (group 3). CONCLUSION: In noncirrhotic HCC patients, histological steatosis was frequently present, whereas overt steatohepatitis did not occur. These findings may be relevant for HCC pathogenesis in NAFLD.

Published
2016

47. Short article: Management of ruptured hepatocellular carcinoma in a European tertiary care center

Author

Rijckborst, V., Borg, M.J. Ter, Tjwa, E.T., Sprengers, D., Verhoef, K., Moelker, A., Ijzermans, J.N., Man, R.A. de, Rijckborst, V., Borg, M.J. Ter, Tjwa, E.T., Sprengers, D., Verhoef, K., Moelker, A., Ijzermans, J.N., and Man, R.A. de

Abstract

Item does not contain fulltext, GOALS AND BACKGROUND: Spontaneous rupture is a rare complication of hepatocellular carcinoma (HCC). Treatment options consist of transcatheter arterial embolization (TAE), hepatic resection, and conservative therapy. The best approach is under debate. STUDY: This study presents a review of clinical data of patients with a ruptured HCC admitted to a European tertiary care center. RESULTS: Eleven patients were included; six (55%) had underlying cirrhosis. The majority of patients (73%) had no previous history of HCC. Spontaneous HCC rupture was diagnosed using abdominal computed tomography with or without a diagnostic paracentesis. Computed tomography showed one or two tumors in eight (73%) patients; the other patients had multiple tumors or diffuse infiltrative HCC. Seven (64%) patients were initially treated by TAE and one (9%) patient underwent hepatic resection. The remaining three (27%) patients, all of whom had liver cirrhosis, received conservative therapy. Two patients initially treated by TAE underwent a delayed resection and ultimately received systemic therapy. Overall, at the end of the follow-up period, three patients were still alive at 84, 991, and 1026 days after the initial presentation. Eight (73%) patients had died after a median of 88 days (range 7-417). One year after presentation, none of the conservatively treated patients was alive compared with three out of seven (43%) patients treated with TAE with or without delayed resection. CONCLUSION: Patients with a spontaneously ruptured HCC have a poor prognosis. In selected patients, however, prolonged survival is possible using TAE as initial therapy with or without a delayed resection and systemic therapy.

Published
2016

49. Rapid hepatic clearance of full length CCN-2/CTGF: a putative role for LRP1-mediated endocytosis

Author

Gerritsen, K.G. (Karin), Bovenschen, N. (N.), Nguyen, T.Q. (Tri), Sprengers, D. (Dave), Koeners, M.P. (Maarten), van Koppen, A.N., Joles, J.A. (Jaap), Goldschmeding, R. (Roel), Kok, R.J. (Robbert), Gerritsen, K.G. (Karin), Bovenschen, N. (N.), Nguyen, T.Q. (Tri), Sprengers, D. (Dave), Koeners, M.P. (Maarten), van Koppen, A.N., Joles, J.A. (Jaap), Goldschmeding, R. (Roel), and Kok, R.J. (Robbert)

Abstract

CCN-2 (connective tissue growth factor; CTGF) is a key factor in fibrosis. Plasma CCN-2 has biomarker potential in numerous fibrotic disorders, but it is unknown which pathophysiological factors determine plasma CCN-2 levels. The proteolytic amino-terminal fragment of CCN-2 is primarily eliminated by the kidney. Here, we investigated elimination and distribution profiles of full length CCN-2 by intravenous administration of recombinant CCN-2 to rodents. After bolus injection in mice, we observed a large initial distribution volume (454 mL/kg) and a fast initial clearance (120 mL/kg/min). Immunosorbent assay and immunostaining showed that CCN-2 distributed mainly to the liver and was taken up by hepatocytes. Steady state clearance in rats, determined by continuous infusion of CCN-2, was fast (45 mL/kg/min). Renal CCN-2 clearance, determined by arterial and renal vein sampling, accounted for only 12 % of total clearance. Co-infusion of CCN-2 with receptor-associated protein (RAP), an antagonist of LDL-receptor family proteins, showed that RAP prolonged CCN-2 half-life and completely prevented CCN-2 internalization by hepatocytes. This suggests that hepatic uptake of CCN-2 is mediated by a RAP-sensitive mechanism most likely involving LRP1, a member of the LDL-receptor family involved in hepatic clearance of various plasma proteins. Surface plasmon resonance binding studies confirmed that CCN-2 is an LRP1 ligand. Co-infusion of CCN-2 with an excess of the heparan sulphate-binding protamine lowered the large initial distribution volume of CCN-2 by 88 % and reduced interstitial staining of CCN-2, suggesting binding of CCN-2 to heparan sulphate proteoglycans (HSPGs). Protamine did not affect clearance rate, indicating that RAP-sensitive clearance of CCN-2 is HSPG independent. In conclusion, unlike its amino-terminal fragment which is cleared by the kidney, ful

Published
2016
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50. Cross talk between nucleotide synthesis pathways with cellular immunity in constraining hepatitis e virus replication

Author

Wang, Y. (Yijin), Wang, W. (Wenshi), Xu, L. (Lei), Zhou, X. (Xinying), Shokrollahi, E. (Ehsan), Felczak, K. (K.), Laan, L.J.W. (Luc) van der, Pankiewicz, K.W. (Krzysztof W.), Sprengers, D. (Dave), Raat, N.J.H. (Nicolaas), Metselaar, H.J. (Herold), Peppelenbosch, M.P. (Maikel), Pan, Q. (Qiuwei), Wang, Y. (Yijin), Wang, W. (Wenshi), Xu, L. (Lei), Zhou, X. (Xinying), Shokrollahi, E. (Ehsan), Felczak, K. (K.), Laan, L.J.W. (Luc) van der, Pankiewicz, K.W. (Krzysztof W.), Sprengers, D. (Dave), Raat, N.J.H. (Nicolaas), Metselaar, H.J. (Herold), Peppelenbosch, M.P. (Maikel), and Pan, Q. (Qiuwei)

Abstract

iruses are solely dependent on host cells to propagate; therefore, understanding virus-host interaction is important for antiviral drug development. Since de novo nucleotide biosynthesis is essentially required for both host cell metabolism and viral replication, specific catalytic enzymes of these pathways have been explored as potential antiviral targets. In this study, we investigated the role of different enzymatic cascades of nucleotide biosynthesis in hepatitis E virus (HEV) replication. By profiling various pharmacological inhibitors of nucleotide biosynthesis, we found that targeting the early steps of the purine biosynthesis pathway led to the enhancem

Published
2016
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