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5. Novel α-1,3-Glucosyltransferase Variants and Their Broad Clinical Polycystic Liver Disease Spectrum.

Author

Boerrigter, Melissa M., te Morsche, René H. M., Venselaar, Hanka, Pastoors, Nikki, Geerts, Anja M., Hoorens, Anne, and Drenth, Joost P. H.

Subjects
ARACHNOID cysts, LIVER diseases, CYSTIC kidney disease, THREE-dimensional modeling, KIDNEY physiology
Abstract

Protein-truncating variants in α-1,3-glucosyltransferase (ALG8) are a risk factor for a mild cystic kidney disease phenotype. The association between these variants and liver cysts is limited. We aim to identify pathogenic ALG8 variants in our cohort of autosomal dominant polycystic liver disease (ADPLD) individuals. In order to fine-map the phenotypical spectrum of pathogenic ALG8 variant carriers, we performed targeted ALG8 screening in 478 ADPLD singletons, and exome sequencing in 48 singletons and 4 patients from two large ADPLD families. Eight novel and one previously reported pathogenic variant in ALG8 were discovered in sixteen patients. The ALG8 clinical phenotype ranges from mild to severe polycystic liver disease, and from innumerable small to multiple large hepatic cysts. The presence of <5 renal cysts that do not affect renal function is common in this population. Three-dimensional homology modeling demonstrated that six variants cause a truncated ALG8 protein with abnormal functioning, and one variant is predicted to destabilize ALG8. For the seventh variant, immunostaining of the liver tissue showed a complete loss of ALG8 in the cystic cells. ALG8-associated ADPLD has a broad clinical spectrum, including the possibility of developing a small number of renal cysts. This broadens the ADPLD genotype–phenotype spectrum and narrows the gap between liver-specific ADPLD and kidney-specific ADPKD. [ABSTRACT FROM AUTHOR]

Published
2023
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6. Tamoxifen for the treatment of polycystic liver disease

Author

Aapkes, Sophie E., Bernts, Lucas H.P., van den Berg, M., Gansevoort, Ron T., and Drenth, Joost P.H.

Subjects
tamoxifen, Antineoplastic Agents, Hormonal, Cysts, Liver Diseases, Middle Aged, polycystic liver disease, estrogen, Humans, Female, Clinical Case Report, case-report, Tomography, X-Ray Computed, Research Article, hepatic cyst, Follow-Up Studies
Abstract

Rationale: Polycystic liver disease is a rare disease characterized by the growth of numerous cysts in the liver. The liver function remains well preserved, but liver volumes can grow very large, and some patients ultimately need a liver transplantation. Other treatment options are limited and there is an unmet need for new therapeutic options. Patient concerns: We describe a 59-year-old patient with pain in the abdomen, especially when bending forward. Five years ago, she was diagnosed with breast cancer and as an incidental finding a couple of large liver cysts were diagnosed, explaining her abdominal pain. Diagnosis: Polycystic liver disease with several large liver cysts. Interventions: The patient was treated with tamoxifen, an estrogen receptor modulator, as treatment for her hormone receptor positive breast cancer. One of the liver cysts was aspirated. Outcomes: In the 4.6 years after the start of tamoxifen treatment, 20 mg once daily, the volume of her liver cysts decreased remarkably. There was a reduction of combined cyst volume from 311 mL to 22 mL without percutaneous drainage. Lessons: Epidemiological as well as experimental evidence supports a pivotal role for estrogens as a driver for growth of polycystic livers. Estrogen antagonism has often been proposed as a therapeutic target, but supporting evidence is lacking in the literature. We hypothesize that the decrease in cyst size in this patient was caused by tamoxifen therapy, suggesting an in vivo antagonistic effect on cystic cholangiocytes. This is an important finding because tamoxifen could be a promising new treatment option for polycystic liver disease.

Published
2021

7. Complexity and Specificity of Sec61-Channelopathies: Human Diseases Affecting Gating of the Sec61 Complex

Author

Sicking, Mark, Lang, Sven, Bochen, Florian, Roos, Andreas, Drenth, Joost P. H., Zakaria, Muhammad, Zimmermann, Richard, and Linxweiler, Maximilian

Subjects
BiP, QH301-705.5, Medizin, common variable immunodeficiency, Review, Sec63, Sec62, polycystic liver disease, congenital disorder of glycosylation, endoplasmic reticulum, Renal disorders Radboud Institute for Molecular Life Sciences [Radboudumc 11], Allosteric Regulation, Neoplasms, Sec61-channelopathies, Humans, neutropenia, Channelopathies, Biology (General), Endoplasmic Reticulum Chaperone BiP, Ion Channel Gating, SSR/TRAP complex, Heat-Shock Proteins, SEC Translocation Channels
Abstract

Contains fulltext : 235606.pdf (Publisher’s version ) (Open Access) The rough endoplasmic reticulum (ER) of nucleated human cells has crucial functions in protein biogenesis, calcium (Ca(2+)) homeostasis, and signal transduction. Among the roughly one hundred components, which are involved in protein import and protein folding or assembly, two components stand out: The Sec61 complex and BiP. The Sec61 complex in the ER membrane represents the major entry point for precursor polypeptides into the membrane or lumen of the ER and provides a conduit for Ca(2+) ions from the ER lumen to the cytosol. The second component, the Hsp70-type molecular chaperone immunoglobulin heavy chain binding protein, short BiP, plays central roles in protein folding and assembly (hence its name), protein import, cellular Ca(2+) homeostasis, and various intracellular signal transduction pathways. For the purpose of this review, we focus on these two components, their relevant allosteric effectors and on the question of how their respective functional cycles are linked in order to reconcile the apparently contradictory features of the ER membrane, selective permeability for precursor polypeptides, and impermeability for Ca(2+). The key issues are that the Sec61 complex exists in two conformations: An open and a closed state that are in a dynamic equilibrium with each other, and that BiP contributes to its gating in both directions in cooperation with different co-chaperones. While the open Sec61 complex forms an aqueous polypeptide-conducting- and transiently Ca(2+)-permeable channel, the closed complex is impermeable even to Ca(2+). Therefore, we discuss the human hereditary and tumor diseases that are linked to Sec61 channel gating, termed Sec61-channelopathies, as disturbances of selective polypeptide-impermeability and/or aberrant Ca(2+)-permeability.

Published
2021

9. Abdominal wall hernia is a frequent complication of polycystic liver disease and associated with hepatomegaly.

Author

Barten, Thijs R. M., Bökkerink, Roos‐Anne M. P., Venderink, Wulphert, Gevers, Tom J. G., ten Broek, Richard P. G., and Drenth, Joost P. H.

Subjects
HERNIA, ABDOMINAL wall, LIVER diseases, HEPATOMEGALY, UMBILICAL hernia
Abstract

Background and Aim: Polycystic liver disease (PLD) is related to hepatomegaly which causes an increased mechanical pressure on the abdominal wall. This may lead to abdominal wall herniation (AWH). We set out to establish the prevalence of AWH in PLD and explore risk factors. Methods: In this cross‐sectional cohort study, we assessed the presence of AWHs from PLD patients with at least 1 abdominal computed tomography or magnetic resonance imaging scan. AWH presence on imaging was independently evaluated by two researchers. Data on potential risk factors were extracted from clinical files. Results: We included 484 patients of which 40.1% (n = 194) had an AWH. We found a clear predominance of umbilical hernias (25.8%, n = 125) while multiple hernias were present in 6.2% (n = 30). Using multivariate analysis, male sex (odds ratio [OR] 2.727 p <.001), abdominal surgery (OR 2.575, p <.001) and disease severity according to the Gigot classification (Type 3 OR 2.853, p <.001) were identified as risk factors. Height‐adjusted total liver volume was an independent PLD‐specific risk factor in the subgroup of patients with known total liver volume (OR 1.363, p =.001). Patients with multiple hernias were older (62.1 vs. 55.1, p =.001) and more frequently male (22.0% vs. 50.0%, p =.001). Conclusion: AWHs occur frequently in PLD with a predominance of umbilical hernias. Hepatomegaly is a clear disease‐specific risk factor. [ABSTRACT FROM AUTHOR]

Published
2022
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10. Estrogens in polycystic liver disease: A target for future therapies?

Author

Aapkes, Sophie E., Bernts, Lucas H. P., Barten, Thijs R. M., van den Berg, Marjan, Gansevoort, Ron T., and Drenth, Joost P. H.

Subjects
LIVER diseases, ESTROGEN, ESTROGEN receptors, HORMONE therapy, HOT flashes, QUALITY of life
Abstract

Background and Aims: Patients suffering from polycystic liver disease (PLD) can develop large liver volumes, leading to physical and psychological complaints, reducing quality of life. There is an unmet need for new therapies in these patients. Estrogen seems to be a promising target for new therapies. In this review, we summarize the available experimental and epidemiological evidence to unravel the role of estrogens and other female hormones in PLD, to answer clinical questions and identify new targets for therapy. Methods: We identified all experimental and epidemiologial studies concerning estrogens or other female hormones and PLD, to answer pre‐defined clinial questions. Results: Female sex is the most important risk factor for the presence and severity of disease; estrogen supplementation enhances liver growth and after menopause, liver growth decreases. Experimental studies show the presence of the estrogen receptors alfa and beta on cystic cholangiocytes, and increased in vitro growth after administration of estrogen. Conclusions: Based on the available evidence, female PLD patients should be discouraged from taking estrogen‐containing contraceptives or hormone replacement therapy. Since liver growth rates decline after menopause, treatment decisions should be based on measured liver growth in postmenopausal women. Finally, blockage of estrogen receptors or estrogen production is a promising target for new therapies. [ABSTRACT FROM AUTHOR]

Published
2021
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11. Rationale and design of the RESOLVE trial: lanreotide as a volume reducing treatment for polycystic livers in patients with autosomal dominant polycystic kidney disease

Author

Gevers Tom JG, Chrispijn Melissa, Wetzels Jack FM, and Drenth Joost PH

Subjects
ADPKD, Urinary biomarkers, Polycystic liver disease, Lanreotide, Diseases of the genitourinary system. Urology, RC870-923
Abstract

Abstract Background A large proportion of patients with autosomal dominant polycystic kidney disease (ADPKD) suffers from polycystic liver disease. Symptoms arise when liver volume increases. The somatostatin analogue lanreotide has proven to reduce liver volume in patients with polycystic liver disease. However, this study also included patients with isolated polycystic liver disease (PCLD). The RESOLVE trial aims to assess the efficacy of lanreotide treatment in ADPKD patients with symptomatic polycystic livers. In this study we present the design of the RESOLVE trial. Methods/design This open-label clinical trial evaluates the effect of 6 months of lanreotide in ADPKD patients with symptomatic polycystic livers. Primary outcome is change in liver volume determined by computerised tomography-volumetry. Secondary outcomes are changes in total kidney volume, kidney intermediate volume and renal function. Furthermore, urinary (NGAL, α1-microglobulin, KIM-1, H-FABP, MCP-1) and serum (fibroblast growth factor 23) biomarkers associated with ADPKD disease severity are assessed to investigate whether these biomarkers predict treatment responses to lanreotide. Moreover, safety and tolerability of the drug in ADPKD patients will be assessed. Discussion We anticipate that lanreotide is an effective therapeutic option for ADPKD patients with symptomatic polycystic livers and that this trial aids in the identification of patient related factors that predict treatment response. Trial registration number Clinical trials.gov NCT01354405

Published
2012
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12. Management of portal hypertension and ascites in polycystic liver disease.

Author

Bernts, Lucas H. P., Drenth, Joost P. H., and Tjwa, Eric T. T. L.

Subjects
*BUDD-Chiari syndrome, *LIVER diseases, *ASCITES, *PORTAL hypertension, *PORTAL vein, *MAGNETIC resonance imaging
Abstract

Patients suffering from polycystic liver disease may develop Hepatic Venous Outflow Obstruction, Portal Vein Obstruction and/or Inferior Caval Vein Syndrome because of cystic mass effect. This can cause portal hypertension, leading to ascites, variceal haemorrhage or splenomegaly. For this review, we evaluate the evidence to provide clinical guidance for physicians faced with this complication. Diagnosis is made with imaging such as ultrasound, computed tomography or magnetic resonance imaging. Therapy includes conventional therapy with diuretics and paracentesis, and medical therapy using somatostatin analogues. Based on disease phenotype various (non‐)surgical liver‐volume reducing therapies, hepatic or portal venous stenting, transjugular intrahepatic portosystemic shunts and liver transplantation may be considered. Because of complicated anatomy, use of high‐risk interventions and lack of empirical evidence, patients should be treated in expert centres. [ABSTRACT FROM AUTHOR]

Published
2019
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13. Severity in polycystic liver disease is associated with aetiology and female gender: Results of the International PLD Registry.

Author

Aerts, René M. M., Kievit, Wietske, Jong, Michiel E., Drenth, Joost P. H., Ahn, Curie, Bañales, Jesús M., Reiterová, Jana, and Nevens, Frederik

Subjects
GENETIC disorders, LIVER diseases
Abstract

Background & Aims: Polycystic liver disease (PLD) occurs in two genetic disorders, autosomal‐dominant polycystic kidney disease (ADPKD) and autosomal‐dominant polycystic liver disease (ADPLD). The aim of this study is to compare disease severity between ADPKD and ADPLD by determining the association between diagnosis and height‐adjusted total liver volume (hTLV). Methods: We performed a cross‐sectional analysis with hTLV as endpoint. Patients were identified from the International PLD Registry (>10 liver cysts) and included in our analysis when PLD diagnosis was made prior to September 2017, hTLV was available before volume‐reducing therapy (measured on computed tomography or magnetic resonance imaging) and when patients were tertiary referred. Data from the registry were retrieved for age, diagnosis (ADPKD or ADPLD), gender, height and hTLV. Results: A total of 360 patients (ADPKD n = 241; ADPLD n = 119) met our inclusion criteria. Female ADPKD patients had larger hTLV compared with ADPLD (P = 0.008). In a multivariate regression analysis, ADPKD and lower age at index CT were independently associated with larger hTLV in females, whereas in males a higher age was associated with larger hTLV. Young females (≤51 years) had larger liver volumes compared with older females (>51 years) in ADPKD. Conclusion: Aetiology is presented as a new risk factor associated with PLD severity. Young females with ADPKD represent a subgroup of PLD patients with the most severe phenotype expressed in hTLV. [ABSTRACT FROM AUTHOR]

Published
2019
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14. Excellent survival after liver transplantation for isolated polycystic liver disease: an European Liver Transplant Registry study

Author

van Keimpema, Loes, Nevens, Frederik, Adam, Rene, Porte, Robert J., Fikatas, Panagiotis, Becker, Thomas, Kirkegaard, Preben, Metselaar, Herold J., Drenth, Joost P. H., and Groningen Institute for Organ Transplantation (GIOT)

Subjects
polycystic liver disease, FENESTRATION, liver transplantation, treatment, KIDNEY-TRANSPLANTATION, VOLUME, MANAGEMENT, Membrane transport and intracellular motility [NCMLS 5], liver cyst, CYSTS, Molecular gastro-enterology and hepatology [IGMD 2]
Abstract

Item does not contain fulltext Patients with end-stage isolated polycystic liver disease (PCLD) suffer from incapacitating symptoms because of very large liver volumes. Liver transplantation (LT) is the only curative option. This study assesses the feasibility of LT in PCLD. We used the European Liver Transplant Registry (ELTR) database to extract demographics and outcomes of 58 PCLD patients. We used Kaplan-Meier survival analysis for survival rates. Severe abdominal pain (75%) was the most prominent symptom, while portal hypertension (35%) was the most common complication in PCLD. The explantation of the polycystic liver was extremely difficult in 38% of patients, because of presence of adhesions from prior therapy (17%). Karnofsky score following LT was 90%. The 1- and 5-year graft survival rate was 94.3% and 87.5%, while patient survival rate was 94.8% and 92.3%, respectively. Survival rates after LT for PCLD are good.

Published
2011

15. The Association of Combined Total Kidney and Liver Volume with Pain and Gastrointestinal Symptoms in Patients with Later Stage Autosomal Dominant Polycystic Kidney Disease.

Author

D'agnolo, Hedwig M.a., Casteleijn, Niek F., Gevers, Tom J.G., de Fijter, Hans, van Gastel, Maartje D.a., Messchendorp, annemarie L., Peters, Dorien J.M., Salih, Mahdi, Soonawala, Darius, Spithoven, Edwin M., Visser, Folkert W., Wetzels, Jack F.M., Zietse, Robert, Gansevoort, Ron T., and Drenth, Joost P.H.

Subjects
GASTROINTESTINAL diseases, POLYCYSTIC kidney disease, PAIN, LIVER, SYMPTOMS, GLOMERULAR filtration rate, ABDOMINAL pain, ANTHROPOMETRY, BIOLOGICAL models, COMPARATIVE studies, DEGLUTITION disorders, KIDNEYS, MAGNETIC resonance imaging, RESEARCH methodology, MEDICAL cooperation, RESEARCH, EVALUATION research, PAIN measurement, RANDOMIZED controlled trials, DISEASE complications
Abstract

Background: There is an ongoing debate if and how kidney and liver volume are associated with pain and gastrointestinal (GI) symptoms in autosomal dominant polycystic kidney disease (ADPKD) patients. Since both kidney and liver volume could interact, we investigated whether combined total kidney and liver volume had stronger associations with ADPKD-related pain and GI symptoms than the volumes of the organs separately.Methods: We used baseline data from the DIPAK-1 study, which included ADPKD patients with an estimated glomerular filtration rate (eGFR) between 30 and 60 mL/min/1.73 m2. MR imaging was performed to measure height-adjusted total kidney volume (hTKV), height-adjusted total liver volume (hTLV) and the combination of both (height-adjusted total kidney liver volume [hTKLV]).Results: Three hundred nine ADPKD patients were included with a mean age of 48 ± 7 years, 53% female, eGFR 50 ± 11 mL/min/1.73 m2 and median hTKV, hTLV and hTKLV of 1,095 (758-1,669), 1,173 (994-1,523) and 2,496 (1,972-3,352) mL/m, respectively. ADPKD-related pain and GI symptoms were present in, respectively, 27.5 and 61.2% of patients. Gender was no effect modifier in the association between kidney and/or liver volume, and symptom burden, indicating that all models could be tested in the overall study population. hTKLV and hTLV were significantly associated with pain and GI symptoms, whereas hTKV was not. Model testing revealed that the associations of pain and GI symptoms with hTKLV were significantly stronger than with hTKV (p = 0.04 and p = 0.04, respectively) but not when compared to hTLV (p = 0.2 and p = 0.5, respectively).Conclusions: This study indicates that combined kidney and liver volume was associated with the presence and severity of pain and GI symptoms in ADPKD, with a more prominent role for hTLV than for hTKV. [ABSTRACT FROM AUTHOR]

Published
2017
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16. Center is an important indicator for choice of invasive therapy in polycystic liver disease.

Author

D'Agnolo, Hedwig M. A., Kievit, Wietske, Munster, Kim N., Laan, Jouke J. H., Nevens, Frederik, and Drenth, Joost P. H.

Subjects
LIVER disease treatment, SCLEROTHERAPY, POLYCYSTIC kidney disease, MULTIVARIATE analysis, LIVER transplantation, DIAGNOSIS
Abstract

Polycystic liver disease ( PLD) is a rare genetic disorder with progressive cyst growth as the primary phenotype. Therapy consists of volume reduction through invasive surgical or radiological procedures. To understand the process of treatment decision, our aim was to identify factors that increased the likelihood of treatment. We performed a cross-sectional study using an international population of patients with PLD. We collected data on the following therapies: liver transplantation, resection, fenestration, and aspiration sclerotherapy. Data on the potential determinants, sex, center, autosomal dominant polycystic kidney disease ( ADPKD), autosomal dominant polycystic liver disease ( ADPLD), age at diagnosis, symptoms, and phenotype, were included. We corrected for follow-up time. We included 578 patients in our study, and 35% underwent invasive therapy. Multivariate regression analysis showed that number of symptoms and age at diagnosis of PLD increased the likelihood of treatment (respectively, RR: 1.4, P < 0.001 and RR = 1.4, P = 0.03). The choice for liver transplantation or aspiration sclerotherapy was center dependent ( RR: 0.7, P < 0.001 and RR: 1.1, P = 0.03, respectively). The results of our international cross-sectional study suggest that a higher number of symptoms and every 10 years of PLD diagnosis increase the risk to undergo treatment by 40%. The choice to elect a particular modality is center dependent. [ABSTRACT FROM AUTHOR]

Published
2017
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17. Effect of lanreotide on polycystic liver and kidneys in autosomal dominant polycystic kidney disease: an observational trial.

Author

Gevers, Tom J.G., Hol, Jeroen C., Monshouwer, René, Dekker, Helena M., Wetzels, Jack F.M., and Drenth, Joost P.H.

Subjects
POLYCYSTIC kidney disease treatment, LIVER disease treatment, SOMATOSTATIN receptors, GLOMERULAR filtration rate, QUALITY of life, MANAGEMENT
Abstract

Background & Aim Several trials have demonstrated that somatostatin analogues decrease liver volume in mixed populations of patients with autosomal dominant polycystic kidney disease ( ADPKD) and isolated polycystic liver disease. Chronic renal dysfunction in ADPKD may affect treatment efficacy of lanreotide and possibly enhances risk for adverse events. The aim of this open-label clinical trial ( RESOLVE trial) was to assess the efficacy of 6-month lanreotide treatment, 120 mg, subcutaneously every 4 weeks in ADPKD patients with symptomatic polycystic liver disease. Methods Primary outcome was change in liver volume after 6 months; secondary outcomes were changes in kidney volume, estimated glomerular filtration rate ( eGFR), symptom relief and health-related quality of life (Euro-Qol5D). We excluded patients with an eGFR <30 ml/min/1.73 m2. We used the Wilcoxon signed-rank test or paired two-sided t-test to analyze within-group differences. Results We included 43 ADPKD patients with polycystic liver disease (84% female, median age 50 years, mean eGFR 63 ml/min/1.73 m2). Median liver volume decreased from 4859 ml to 4595 ml (−3.1%; P < 0.001), and median kidney volume decreased from 1023 ml to 1012 ml (−1.7%; P = 0.006). eGFR declined 3.5% after the first injection, remained stable up to study end, to decline again after lanreotide withdrawal. Lanreotide significantly relieved post-prandial fullness, shortness of breath and abdominal distension. Three participants had a suspected episode of hepatic or renal cyst infection during this study. Conclusion Lanreotide reduced polycystic liver and kidney volumes and decreases symptoms in ADPKD patients. Moreover, eGFR decreased acutely after starting lanreotide, stabilized thereafter and declined again after withdrawal. Trial registration number: Clinical trials.gov NCT01354405 (Registration: 13 May 2011). [ABSTRACT FROM AUTHOR]

Published
2015
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18. Aspiration sclerotherapy combined with pasireotide to improve reduction of large symptomatic hepatic cysts (SCLEROCYST): study protocol for a randomized controlled trial.

Author

Wijnands, Titus F. M., Gevers, Tom J. G., Kool, Leo J. Schultze, and Drenth, Joost P. H.

Subjects
RESPIRATORY aspiration, SCLEROTHERAPY, MEDICAL suction, CYSTS (Pathology), TUMORS
Abstract

Background: Aspiration sclerotherapy is an effective therapeutic option for large symptomatic hepatic cysts. However, incomplete cyst reduction following aspiration sclerotherapy is frequently reported. Strong post-procedural cyst fluid secretion by cholangiocytes, which line the epithelium of the hepatic cyst, seems to be associated with lower reduction rates. Previous studies showed that somatostatin analogues curtail hepatic cyst fluid production. This trial will evaluate the effect of aspiration sclerotherapy combined with the somatostatin analogue pasireotide on cyst reduction. By combining treatment modalities we aim to improve cyst reduction leading to greater symptomatic relief and reduced rates of cyst recurrence. Methods/Design: This single center, randomized, double-blind, placebo-controlled clinical trial evaluates the additional effect of pasireotide when combined with aspiration sclerotherapy in patients with a large (>5 cm) symptomatic hepatic cyst. A total of 34 participants will be randomized in a 1:1 ratio. In the active arm, patients will receive pasireotide (long-acting release, 60 mg injection) two weeks prior to and two weeks following aspiration sclerotherapy. Patients in the control arm will receive placebo injections at corresponding intervals. The primary outcome is proportional cyst diameter reduction four weeks after aspiration sclerotherapy compared to baseline measurements, obtained by ultrasonography. As secondary outcomes, proportional volume reduction, recurrence, symptomatic relief and improvement of health-related quality of life will be assessed. Furthermore, safety and tolerability of the combination of pasireotide and aspiration sclerotherapy will be evaluated. Discussion: This trial aims to improve efficacy of aspiration sclerotherapy by a combined approach of two treatment modalities. We hypothesize that pasireotide will decrease fluid re-accumulation after aspiration sclerotherapy, leading to effective hepatic cyst reduction and symptomatic relief. [ABSTRACT FROM AUTHOR]

Published
2015
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19. Evaluating health-related quality of life in patients with polycystic liver disease and determining the impact of symptoms and liver volume.

Author

Wijnands, Titus F. M., Neijenhuis, Myrte K., Kievit, Wietske, Nevens, Frederik, Hogan, Marie C., Torres, Vicente E., Gevers, Tom J. G., and Drenth, Joost P. H.

Abstract

Background & Aims: Polycystic liver disease (PLD) follows a progressive course ultimately leading to severe hepatomegaly and mechanical complaints in a subset of patients. It is still unknown to what extent this compromises health-related quality of life (HRQL). Our aim was to determine HRQL in PLD patients and investigate its association with concurrent abdominal symptoms and liver volume. Methods: Pooled data of 92 severe PLD patients from two randomized clinical trials were used for our cross-sectional analysis. HRQL was assessed using the generic short-form health survey (SF- 36) resulting in eight scale scores and the summarizing physical (PCS) and mental component score (MCS). Subsequently, these were compared with the general population. Abdominal symptoms were measured with a standardized, 7-point scale questionnaire in 54 patients. We dichotomized symptoms for absence or presence and compared them with the component scores. Finally, a possible correlation between liver volume and HRQL was explored. Results: Demographics showed severe polycystic livers (mean 4906 ± 2315 ml). PCS was significantly lower compared with the general population (P < 0.001), in contrast with a similar MCS (P = 0.82). PLD patients had statistically significant (P < 0.05) diminished physical functioning, role physical, general health, vitality and social functioning scores. Upper- and lower abdominal pain and dyspnoea were significantly associated with a reduced PCS (P < 0.01). No correlation was found between liver volume and HRQL. Conclusion: Polycystic liver disease patients had significantly lower HRQL in the physical dimension compared with the general population. Abdominal pain and dyspnoea had a significant impact on this physical dimension of HRQL. [ABSTRACT FROM AUTHOR]

Published
2014
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20. Patients with isolated polycystic liver disease referred to liver centres: clinical characterization of 137 cases.

Author

Van Keimpema, Loes, De Koning, Daan B., Van Hoek, Bart, Van Den Berg, Aad P., Van Oijen, Martijn G. H., De Man, Robert A., Nevens, Frederik, and Drenth, Joost P. H.

Subjects
LIVER diseases, CYSTS (Pathology), GENETIC mutation, WOMEN patients, REFERRAL centers (Information services), DISEASES, PATIENTS
Abstract

Isolated polycystic liver disease (PCLD) is characterized by the presence of multiple cysts in the liver in the absence of polycystic kidneys. The clinical profile of PCLD is poorly defined and we set up a study for the clinical characteristics of PCLD. We collected clinical data on 188 PCLD patients (defined as >10 liver cysts) from five tertiary referral centres, and 137 patients were selected for the purpose of this study. We performed molecular analysis of the PCLD associated genes PRKCSH and SEC63 in 91 patients. A total of 118 (86%) patients were female. The majority of patients (88%) had >20 cysts. The median age at diagnosis was 47 years (range 23-84). 37 (41%) patients carried a mutation. Clinical symptoms at presentation were present in 111 (84%) patients. γ-glutamyl transferase was elevated to 1.4 times upper limit of normal (interquartile range 1.0-2.7). The presence of a mutation and female gender predicted a more severe course: female patients were 9 years younger at the time of diagnosis (47 years; range 23-84) and 91% had symptoms ( P<0.01); likewise, mutation carriers were younger at presentation (39 years; range 35-48) and 95% of this cohort had symptoms ( P<0.01). During follow-up [median 8.2 years (range 0-35)], 10% of untreated and 51% of treated patients developed complications. Mortality in this cohort was 8%, but only 2% died of PCLD-related causes. 58% of patients were treated a median of 2 years (range 0-25) after diagnosis. Symptomatic PCLD patients are mainly females. Females and mutation carriers were younger at diagnosis and had a more severe course of disease. [ABSTRACT FROM AUTHOR]

Published
2011
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21. Carbohydrate antigen 19-9 is extremely elevated in polycystic liver disease.

Author

Waanders, Esm, van Keimpema, Loes, Brouwer, Johannes T., van Oijen, Martijn G. H., Aerts, Raymond, Sweep, Fred C. G. J., Nevens, Frederik, and Drenth, Joost P. H.

Subjects
ANTIGENS, BIOMARKERS, GASTROINTESTINAL diseases, CYSTS (Pathology), LIVER diseases
Abstract

Background/Aims: Carbohydrate antigen 19-9 (CA19-9) is used as a biomarker to differentiate benign from malignant gastrointestinal disorders. We examined the value of CA19-9 measurement in polycystic livers after observing high CA19-9 cyst fluid levels in a benign polycystic liver case. Methods: We determined CA19-9 levels in serum ( n=120) and hepatic cyst fluid ( n=81), from patients with polycystic livers ( n=109) and simple hepatic cysts ( n=24). Further, we analysed CA19-9 expression in normal and polycystic liver tissue ( n=17). Results: Cyst fluid CA19-9 levels from both polycystic livers and simple hepatic cysts were extremely high (median 91 000 U/ml, range 14–15 870 000 U/ml; median 85 000 U/ml, range 332–1 744 000 U/ml respectively). Serum CA19-9 levels were significantly higher in polycystic liver patients (median 30 U/ml, range 0–1200 U/ml) compared with patients with simple hepatic cysts (median 10 U/ml, range 3–200 U/ml, P=0.0011). Serum CA19-9 levels correlated with those in cyst fluid ( r=0.3979, P=0.0399), polycystic liver volume ( r=0.3870, P=0.0025) and the size of the largest cyst (simple cysts group; r=0.5319, P=0.0280). Cyst epithelia showed strong CA19-9 expression. Evacuation of cyst fluid in four patients resulted in a dramatic decrease in the serum CA19-9 levels (60–95%). Conclusions: CA19-9 levels are high in the cyst fluid and serum of polycystic liver disease patients due to production and secretion by cyst epithelia. It does not reflect malignancy in these patients and may be of value as a biomarker for intervention efficiency assessment. [ABSTRACT FROM AUTHOR]

Published
2009
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22. Drug holiday in patients with polycystic liver disease treated with somatostatin analogues.

Author

van Aerts, René M. M., Kolkman, Marieke, Kievit, Wietske, Gevers, Tom J. G., Nevens, Frederik, and Drenth, Joost P. H.

Abstract

Background: Somatostatin analogues (SAs) reduce liver volume and relief symptoms in polycystic liver disease (PLD). Its effect wears off after continuing therapy suggesting development of SA tolerance in patients on chronic therapy. We postulate that a drug holiday resensitizes the liver to its acute pharmacological effects. Therefore, this study examines the liver volume-reducing effect of SAs after a drug holiday. Methods: Patients were identified from the International PLD Registry and included in our analysis when (1) treated with SAs during two cycles separated by a drug holiday and (2) height-adjusted total liver volume (hTLV) was available at start and end of each cycle. For our primary outcome we compared the effect of SAs (in % per 6 months) on hTLV between the first and second treatment cycle. Results: In 34 patients, initial liver volume-reducing effect was similar to that after rechallenge [−2.6% per 6 months (interquartile range, −3.8–0.8) versus −1.6% per 6 months (interquartile range, −3.1–1.1), p = 0.510]. Cessation of treatment led to a rebound effect, but liver volume remained stable compared with the baseline with intermittent therapy in responders to SA [−0.6% (interquartile range, −7.4–5.7) after 46.5 months]. Conclusions: PLD patients treated with SAs benefit from retreatment after a drug holiday. The significant increase of liver volume after cessation of treatment complicates widespread use of a drug holiday as new treatment strategy. Our results contribute to a better understanding of the pharmacological effect of SAs and help to identify patients who might benefit. [ABSTRACT FROM AUTHOR]

Published
2018
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24. A stepwise approach for effective management of chronic pain in autosomal-dominant polycystic kidney disease.

Author

Casteleijn, Niek F., Visser, Folkert W., Drenth, Joost P.H., Gevers, Tom J.G., Groen, Gerbrand J., Hogan, Marie C., and Gansevoort, Ron T.

Subjects
PAIN management, POLYCYSTIC kidney disease, PHYSICAL activity, INTERPERSONAL relations, PATHOLOGICAL physiology, POLYCYSTIC kidney disease treatment, PATIENTS
Abstract

Chronic pain, defined as pain existing for >4–6 weeks, affects >60% of patients with autosomal-dominant polycystic disease (ADPKD). It can have various causes, indirectly or directly related to the increase in kidney and liver volume in these patients. Chronic pain in ADPKD patients is often severe, impacting physical activity and social relationships, and frequently difficult to manage. This review provides an overview of pathophysiological mechanisms that can lead to pain and discusses the sensory innervation of the kidneys and the upper abdominal organs, including the liver. In addition, the results of a systematic literature search of ADPKD-specific treatment options are presented. Based on pathophysiological knowledge and evidence derived from the literature an argumentative stepwise approach for effective management of chronic pain in ADPKD is proposed. [ABSTRACT FROM AUTHOR]

Published
2014

25. Issues in multi-organ transplantation of the liver with kidney or heart in polycystic liver-kidney disease or congenital heart disease: Current practices and immunological aspects.

Author

Taner, Timucin, Hilscher, Moira B., Broda, Christopher R., and Drenth, Joost P.H.

Subjects
*CONGENITAL heart disease, *POLYCYSTIC kidney disease, *LIVER transplantation, *KIDNEY transplantation, *CHRONIC kidney failure
Abstract

Solid organ transplantation has become an integral part of the management of patients with end-stage diseases of the kidney, liver, heart and lungs. Most procedures occur in isolation, but multi-organ transplantation of the liver with either the kidney or heart has become an option. As more patients with congenital heart disease and cardiac cirrhosis survive into adulthood, particularly after the Fontan procedure, liver transplant teams are expected to face questions regarding multi-organ (heart-liver) transplantation. Similarly, patients with polycystic kidneys and livers may be managed by multi-organ transplantation. Herein, we review the indications and outcomes of simultaneous liver-kidney transplantation for polycystic liver-kidney disease, and discuss the indications, timing and procedural aspects of combined heart-liver transplantation. We also summarise the evidence for, and potential mechanisms underlying, the immunoprotective impact of liver allografts on the simultaneously transplanted organs. [ABSTRACT FROM AUTHOR]

Published
2023
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26. Polycystic liver disease: ductal plate malformation and the primary cilium.

Author

Wills, Edgar S., Roepman, Ronald, and Drenth, Joost P.H.

Subjects
*CYSTS (Pathology), *LIVER diseases, *TRANSFORMING growth factors-beta, *CELLULAR signal transduction, *POLYCYSTINS, *CILIA & ciliary motion, *WNT genes
Abstract

Highlights: [•] Recapitulation of the core process of cystogenesis: ductal plate malformation. [•] Reiteration of the roles PRKCSH and SEC63 play in co-translational processing of polycystins. [•] Discussion of signaling pathways Notch, TGF-β, and Wnt in hepatobiliary development. [•] Current overview of the crucial role of the primary cilium in hepatic cystogenesis. [Copyright &y& Elsevier]

Published
2014
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27. Clinical management of polycystic liver disease.

Author

van Aerts, René M.M., van de Laarschot, Liyanne F.M., Banales, Jesus M., and Drenth, Joost P.H.

Subjects
*LIVER diseases, *LIVER tumors, *COMPUTED tomography, *GENETIC testing, *HEPATIC veins
Abstract

Clinical vignette A 41-year old female underwent a computed tomography (CT) scan in 2010 because of symptoms suggestive of appendicitis. Incidentally, multiple liver lesions characterised as cysts were detected. The presence of small to medium sized liver cysts (diameter between <1 cm and 4 cm) in all liver segments (>100 cysts) and absence of kidney cysts in the context of normal renal function led to the clinical diagnosis of autosomal dominant polycystic liver disease (ADPLD). Five years later she was referred to the outpatient clinic with increased abdominal girth, pain in the right upper abdomen and right flank, and early satiety. She had difficulties bending over and could neither cut her toenails nor tie her shoe laces. In her early twenties she had used oral contraception for five years. She has been pregnant twice. Clinical examination showed an enlarged liver reaching into the right pelvic region and crossing the midline of the abdomen. Laboratory testing demonstrated increased gamma-glutamyl transferase (80 IU/L, normal <40 IU/L) and alkaline phosphatase (148 IU/L, normal <100 IU/L) levels. Bilirubin, albumin and coagulation times were within the normal range. A new CT scan in 2015 was compatible with an increased number and size of liver cysts. The diameter of cysts varied between <1 cm and 6 cm (anatomic distribution shown [ Fig. 2 B]). There were no signs of hepatic venous outflow obstruction, portal hypertension or compression on the biliary tract. Height-adjusted total liver volume (htTLV) increased from 2,667 ml/m in 2012 to 4,047 ml/m in 2015 (height 172 cm). The case we present here is not uncommon, and prompts several relevant questions: I. What causes the development of liver cysts? II. Is genetic testing and genetic counselling recommended? III. What is the natural course of polycystic liver disease and what can patients do to stop growth of liver cysts? IV. Which complications may occur during the course of polycystic liver disease? V. What treatment options are currently available? VI. What other potential new and effective therapies will be available in the near future? [ABSTRACT FROM AUTHOR]

Published
2018
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28. Ursodeoxycholic acid in advanced polycystic liver disease: A phase 2 multicenter randomized controlled trial.

Author

D’Agnolo, Hedwig M.A., Kievit, Wietske, Takkenberg, R. Bart, Riaño, Ioana, Bujanda, Luis, Neijenhuis, Myrte K., Brunenberg, Ellen J.L., Beuers, Ulrich, Banales, Jesus M., and Drenth, Joost P.H.

Subjects
*RANDOMIZED controlled trials, *URSODEOXYCHOLIC acid, *LIVER diseases, *POLYCYSTIC kidney disease, *SUBGROUP analysis (Experimental design)
Abstract

Background & Aims Ursodeoxycholic acid (UDCA) inhibits proliferation of polycystic human cholangiocytes in vitro and hepatic cystogenesis in a rat model of polycystic liver disease (PLD) in vivo . Our aim was to test whether UDCA may beneficially affect liver volume in patients with advanced PLD. Methods We conducted an international, multicenter, randomized controlled trial in symptomatic PLD patients from three tertiary referral centers. Patients with PLD and total liver volume (TLV) ⩾2500 ml were randomly assigned to UDCA treatment (15–20 mg/kg/day) for 24 weeks, or to no treatment. Primary endpoint was proportional change in TLV. Secondary endpoints were change in symptoms and health-related quality of life. We performed a post-hoc analysis of the effect of UDCA on liver cyst volume (LCV). Results We included 34 patients and were able to assess primary endpoint in 32 patients, 16 with autosomal dominant polycystic kidney disease (ADPKD) and 16 with autosomal dominant polycystic liver disease (ADPLD). Proportional TLV increased by 4.6 ± 7.7% (mean TLV increased from 6697 ml to 6954 ml) after 24 weeks of UDCA treatment compared to 3.1 ± 3.8% (mean TLV increased from 5512 ml to 5724 ml) in the control group ( p = 0.493). LCV was not different after 24 weeks between controls and UDCA treated patients ( p = 0.848). However, UDCA inhibited LCV growth in ADPKD patients compared to ADPKD controls ( p = 0.049). Conclusions UDCA administration for 24 weeks did not reduce TLV in advanced PLD, but UDCA reduced LCV growth in ADPKD patients. Future studies might explore whether ADPKD and ADPLD patients respond differently to UDCA treatment. Lay summary Current therapies for polycystic liver disease are invasive and have high recurrence risks. Our trial showed that the drug, ursodeoxycholic acid, was not able to reduce liver volume in patients with polycystic liver disease. However, a subgroup analysis in patients that have kidney cysts as well showed that liver cyst volume growth was reduced in patients who received ursodeoxycholic acid in comparison to patients who received no treatment. Trial registration number https://www.clinicaltrials.gov/: NCT02021110. EudraCT Number https://www.clinicaltrialsregister.eu/: 2013-003207-19. [ABSTRACT FROM AUTHOR]

Published
2016
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29. Everolimus does not further reduce polycystic liver volume when added to long acting octreotide: Results from a randomized controlled trial.

Author

Chrispijn, Melissa, Gevers, Tom J.G., Hol, Jeroen C., Monshouwer, Rene, Dekker, Heleen M., and Drenth, Joost P.H.

Subjects
*LIVER diseases, *POLYCYSTIC kidney disease, *HEPATOMEGALY, *SOMATOSTATIN, *QUALITY of life, *RAPAMYCIN, *RANDOMIZED controlled trials
Abstract

Background & Aims: Polycystic liver disease (PLD) is associated with autosomal dominant polycystic kidney disease (ADPKD) or autosomal dominant polycystic liver disease (PCLD). The resulting hepatomegaly compromises quality of life. Somatostatin analogues reduce PLD volume by approximately 5% when given for 6–12months. A pilot trial in 16 ADPKD patients demonstrated that sirolimus, an mTOR inhibitor, reduced PLD volume by 26%. The aim of this study was to assess the PLD volume reducing effect of everolimus and octreotide relative to octreotide monotherapy. Methods: We designed a randomized controlled trial that compared 48weeks of everolimus 2.5mg daily, combined with octreotide 40mg intramuscularly every 4weeks, to octreotide monotherapy. We included PCLD and ADPKD patients. Exclusion criteria were MDRD-GFR <60ml/min/1.73m2 and liver volume <2500ml. Primary outcome was change in liver volume measured with CT-volumetry. Results: We randomized 44 PLD patients (29 PCLD, 15 ADPKD, 89% female) to treatment with octreotide (n=23) or octreotide-everolimus (n=21). Liver volume decreased by 3.5% (p <0.01) in the monotherapy arm, compared to 3.8% with combination therapy (p <0.01). The difference between treatment arms was not significant (p =0.73). Conclusions: Adding everolimus to octreotide in PLD does not increase the liver volume reducing effect of octreotide. [Copyright &y& Elsevier]

Published
2013
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30. Congenital disorders of glycosylation in hepatology: The example of polycystic liver disease

Author

Janssen, Manoe J., Waanders, Esmé, Woudenberg, Jannes, Lefeber, Dirk J., and Drenth, Joost P.H.

Subjects
*CELLULAR pathology, *GENETIC disorders, *GLYCOSYLATION, *HEPATOLOGY, *LIVER diseases, *CHROMOSOME abnormalities, *CYSTS (Pathology), *ENDOPLASMIC reticulum
Abstract

Autosomal dominant polycystic liver disease (PCLD) is a rare progressive disorder characterized by an increased liver volume due to many (>20) fluid-filled cysts of biliary origin. Disease causing mutations in PRKCSH or SEC63 are found in ∼25% of the PCLD patients. Both gene products function in the endoplasmic reticulum, however, the molecular mechanism behind cyst formation remains to be elucidated. As part of the translocon complex, SEC63 plays a role in protein import into the ER and is implicated in the export of unfolded proteins to the cytoplasm during ER-associated degradation (ERAD). PRKCSH codes for the β-subunit of glucosidase II (hepatocystin), which cleaves two glucose residues of Glc3Man9GlcNAc2 N-glycans on proteins. Hepatocystin is thereby directly involved in the protein folding process by regulating protein binding to calnexin/calreticulin in the ER. A separate group of genetic diseases affecting protein N-glycosylation in the ER is formed by the congenital disorders of glycosylation (CDG). In distinct subtypes of this autosomal recessive multisystem disease specific liver symptoms have been reported that overlap with PCLD. Recent research revealed novel insights in PCLD disease pathology such as the absence of hepatocystin from cyst epithelia indicating a two-hit model for PCLD cystogenesis. This opens the way to speculate about a recessive mechanism for PCLD pathophysiology and shared molecular pathways between CDG and PCLD. In this review we will discuss the clinical-genetic features of PCLD and CDG as well as their biochemical pathways with the aim to identify novel directions of research into cystogenesis. [Copyright &y& Elsevier]

Published
2010
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