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Featured researches published by Joanna Ligocka.


Polish Journal of Surgery | 2012

1000 liver transplantations at the Department of General, Transplant and Liver Surgery, Medical University of Warsaw--analysis of indications and results.

Marek Krawczyk; Michał Grąt; Krzysztof Barski; Joanna Ligocka; Arkadiusz Antczak; Oskar Kornasiewicz; Michał Skalski; Waldemar Patkowski; P Nyckowski; K. Zieniewicz; I Grzelak; Jacek Pawlak; Abdulsalam Alsharabi; Tadeusz Wróblewski; Rafał Paluszkiewicz; Bogusław Najnigier; Krzysztof Dudek; Piotr Remiszewski; Piotr Smoter; Mariusz Grodzicki; Michał Korba; Marcin Kotulski; B. Cieślak; Piotr Kalinowski; Piotr Gierej; Mariusz Frączek; Łukasz Rdzanek; Rafał Stankiewicz; Konrad Kobryń; Łukasz Nazarewski

THE AIM OF THE STUDY was to analyze indications and results of the first one thousand liver transplantations at Chair and Clinic of General, Transplantation and Liver Surgery, Medical University of Warsaw. MATERIAL AND METHODS Data from 1000 transplantations (944 patients) performed at Chair and Clinic of General, Transplantation and Liver Surgery between 1994 and 2011 were analyzed retrospectively. These included 943 first transplantations and 55 retransplantations and 2 re-retransplantations. Frequency of particular indications for first transplantation and retransplantations was established. Perioperative mortality was defined as death within 30 days after the transplantation. Kaplan-Meier survival analysis was used to estimate 5-year patient and graft survival. RESULTS The most common indications for first transplantation included: liver failure caused by hepatitis C infection (27.8%) and hepatitis B infection (18%) and alcoholic liver disease (17.7%). Early (< 6 months) and late (> 6 months) retransplantations were dominated by hepatic artery thrombosis (54.3%) and recurrence of the underlying disease (45%). Perioperative mortality rate was 8.9% for first transplantations and 34.5% for retransplantations. Five-year patient and graft survival rate was 74.3% and 71%, respectively, after first transplantations and 54.7% and 52.9%, respectively, after retransplantations. CONCLUSIONS Development of liver transplantation program provided more than 1000 transplantations and excellent long-term results. Liver failure caused by hepatitis C and B infections remains the most common cause of liver transplantation and structure of other indications is consistent with European data.


Annals of Transplantation | 2012

Incidence, pattern and clinical relevance of microbial contamination of preservation fluid in liver transplantation

Michał Grąt; Joanna Ligocka; Zbigniew Lewandowski; Krzysztof Barski; Wacław Hołówko; Michał Skalski; Oskar Kornasiewicz; Paulina Usarek; K. Zieniewicz; Młynarczyk G; Marek Krawczyk

BACKGROUND Transmission of pathogens via preservation fluid (PF) is a potential cause of infection among liver transplant recipients. Here, we evaluated the incidence and pattern of microbial contamination of PF and its impact on postoperative graft function after liver transplantation. MATERIAL/METHODS This longitudinal study included data from 41 primary liver transplantations and 5 re-transplantations performed between December 2010 and September 2011. Results of microbiological analyses of 92 PF samples collected before and after the back-table procedure were evaluated in order to establish the incidence and pattern of contamination. The impact of positive PF cultures on early graft function and rate of pathogen transmission was assessed. Post-transplant antibiotic protocol was based on piperacillin/tazobactam administration for a minimum of 10 days. RESULTS The incidence of contamination was 84.8% (39/46), both for samples collected before and after the back-table procedure. Gram-positive low-virulence organisms typical for superficial saprophytic flora, mainly coagulase-negative staphylococci, were predominant. There were no cases of pathogen transmission from PF to the recipient. Positive cultures of PF samples obtained after the back-table procedure were associated with significant elevation of aspartate (p=0.034) and alanine aminotransferase (p=0.048) on the first 5 postoperative days. No significant differences were found regarding serum bilirubin concentration (p=0.335) and international normalized ratio (p=0.137). CONCLUSIONS Despite high incidence of PF contamination, infections caused by pathogens isolated from PF were not observed. However, presence of pathogens in PF might lead to temporary impairment of graft function.


Annals of Transplantation | 2013

Post-transplant outcomes of patients with and without hepatitis C virus infection according to donor age and gender matching

Michał Grąt; Oskar Kornasiewicz; Zbigniew Lewandowski; Joanna Ligocka; Karolina Grąt; Karolina M. Wronka; K. Zieniewicz; Marek Krawczyk

BACKGROUND The purpose of this study was to evaluate the impact of donor age and donor-recipient gender matching on liver transplantation outcomes, focusing on differences between patients with and without hepatitis C virus (HCV) infection. MATERIAL AND METHODS This retrospective cohort study evaluated 622 liver transplantation recipients. HCV (n=164) and non-HCV (n=458) patients were subdivided by donor age (≤ 30, 31-50, and >50 years) and donor-recipient gender configurations. Five-year patient survival (PS) and graft survival (GS) were set as outcome measures. RESULTS Five-year PS was 83.1% for HCV-positive and 81.6% for HCV-negative patients (p=0.614), with the corresponding GS rates of 81.2% and 79.3% (p=0.538), respectively. In HCV patients, transplantations from donors older than 50 years were associated with lower PS (p=0.035) and GS (p=0.006) than those from donors aged 31-50 years. This difference was not observed among non-HCV recipients (PS, p=0.994; GS, p=0.878). Regarding donor-recipient gender configurations, outcomes were similar in HCV (PS, p=0.751; GS, p=0.592) and non-HCV patients (PS, p=0.217; GS, p=0.249), except for a tendency toward lower PS for male-to-female transplantations than female-to-female transplantations in non-HCV patients (p=0.064). Outcomes of HCV patients were superior to those of non-HCV patients after transplantation from donors aged 31-50 years (PS, p=0.080; GS, p=0.026). CONCLUSIONS Avoiding the transplantation of grafts from donors aged over 50 years to patients with HCV infection might improve the general outcomes of liver transplantation programs. There is no specific rationale for gender matching with respect to HCV status.


Annals of Transplantation | 2015

Relevance of male-to-female sex mismatch in liver transplantation for primary biliary cirrhosis.

Michał Grąt; Zbigniew Lewandowski; Waldemar Patkowski; Karolina M. Wronka; Karolina Grąt; Maciej Krasnodębski; Joanna Ligocka; Hanna Zborowska; Marek Krawczyk

BACKGROUND Because male-to-female transplantations are related to exposure to H-Y antigen, sex matching may influence the outcomes after liver transplantation for autoimmune diseases. The purpose of this retrospective study was to evaluate the relevance of male-to-female mismatch in liver transplantation for primary biliary cirrhosis (PBC). MATERIAL AND METHODS This retrospective study was based on the data of 82 female liver transplant recipients with PBC from a single institution. The primary outcome measure was graft survival at 10 years. The negative effects of well-known risk factors for poor outcomes were evaluated separately and compared between the female-to-female and male-to-female transplantations. RESULTS Graft survival was similar after female-to-female and male-to-female transplantations (74.7% versus 73.1% at 10 years, respectively, p=0.676). Regarding the differential impact of other risk factors, prolonged cold ischemia and increased amount of blood transfusions adversely influenced outcomes after male-to-female transplantation (p=0.039 and p=0.039, respectively) but not after female-to-female transplantation (p=0.843 and p=0.110, respectively). Sex mismatched transplantations were associated with lower 10-year graft survival in subgroups of patients with blood transfusions >4 units (61.4% versus 100.0%, p=0.063) and >8 hours of cold ischemia (54.7% versus 75.8%, p=0.418). CONCLUSIONS Although male-to-female sex mismatch does not seem to yield a direct negative impact on outcomes following liver transplantation for PBC, it can aggravate the negative effects of prolonged cold ischemia and blood transfusions.


Polish Journal of Surgery | 2015

Evolution Of The Results Of 1500 Liver Transplantations Performed In The Department Of General, Transplant And Liver Surgery Medical University Of Warsaw.

Marek Krawczyk; Michał Grąt; Karolina Grąt; Karolina M. Wronka; Maciej Krasnodębski; Jan Stypułkowski; Łukasz Masior; Wacław Hołówko; Joanna Ligocka; P Nyckowski; Tadeusz Wróblewski; Rafał Paluszkiewicz; Waldemar Patkowski; K. Zieniewicz; Leszek Pączek; Piotr Milkiewicz; U. Ołdakowska-Jedynak; Bogusław Najnigier; Krzysztof Dudek; Piotr Remiszewski; I Grzelak; Oskar Kornasiewicz; Marcin Kotulski; Piotr Smoter; Mariusz Grodzicki; Michał Korba; Piotr Kalinowski; Michał Skalski; Krzysztof Zając; Rafał Stankiewicz

UNLABELLED Liver transplantation is a well-established treatment of patients with end-stage liver disease and selected liver tumors. Remarkable progress has been made over the last years concerning nearly all of its aspects. The aim of this study was to evaluate the evolution of long-term outcomes after liver transplantations performed in the Department of General, Transplant and Liver Surgery (Medical University of Warsaw). MATERIAL AND METHODS Data of 1500 liver transplantations performed between 1989 and 2014 were retrospectively analyzed. Transplantations were divided into 3 groups: group 1 including first 500 operations, group 2 including subsequent 500, and group 3 comprising the most recent 500. Five year overall and graft survival were set as outcome measures. RESULTS Increased number of transplantations performed at the site was associated with increased age of the recipients (p<0.001) and donors (p<0.001), increased rate of male recipients (p<0.001), and increased rate of piggyback operations (p<0.001), and decreased MELD (p<0.001), as well as decreased blood (p=0.006) and plasma (p<0.001) transfusions. Overall survival was 71.6% at 5 years in group 1, 74.5% at 5 years in group 2, and 85% at 2.9 years in group 3 (p=0.008). Improvement of overall survival was particularly observed for primary transplantations (p=0.004). Increased graft survival rates did not reach the level of significance (p=0.136). CONCLUSIONS Long-term outcomes after liver transplantations performed in the Department of General, Transplant and Liver Surgery are comparable to those achieved in the largest transplant centers worldwide and are continuously improving despite increasing recipient age and wider utilization of organs procured from older donors.


International Journal of Molecular Sciences | 2017

Decreased Expression of Vitamin D Receptor Affects an Immune Response in Primary Biliary Cholangitis via the VDR-miRNA155-SOCS1 Pathway.

Agnieszka Kempińska-Podhorodecka; Malgorzata Milkiewicz; Urszula Wasik; Joanna Ligocka; Michał Zawadzki; Marek Krawczyk; Piotr Milkiewicz

Primary biliary cholangitis (PBC) is an immune-mediated cholestatic disease. Vitamin D receptor (VDR)-dependent signaling constrains an inflammatory response by targeting the miRNA155-SOCS1 (suppressor of cytokine signaling 1) axis. The VDR-miRNA155-SOCS1 pathway was investigated in the context of the autoimmune response associated with PBC. Human liver tissues from non-cirrhotic PBC (n = 22), cirrhotic PBC (n = 22), cirrhotic primary sclerosing cholangitis (PSC, n = 13), controls (n = 23), and peripheral blood mononuclear cells (PBMC) obtained from PBC (n = 16) and PSC (n = 10) patients and healthy subjects (n = 11) were used for molecular analyses. VDR mRNA and protein expressions were substantially reduced in PBC livers (51% and 59%, respectively). Correspondingly, the decrease of SOCS1 protein expression in PBC livers, after normalization to a marker of lymphocytes and forkhead family transcriptional regulator box P3 (FOXP3, marker of Treg), was observed, and this phenomenon was accompanied by enhanced miRNA155 expression. In PSC livers, protein expressions of VDR and SOCS1 were comparable to the controls. However, in PBM cells, protein expressions of VDR and SOCS1 were considerably decreased in both PBC and PSC. We demonstrated that VDR/miRNA155-modulated SOCS1 expression is decreased in PBC which may lead to insufficient negative regulation of cytokine signaling. These findings suggest that the decreased VDR signaling in PBC could be of importance in the pathogenesis of PBC.


Polish Journal of Surgery | 2013

Short and Long-Term Outcomes After Primary Liver Transplantation in Elderly Patients

Michał Grąt; Oskar Kornasiewicz; Karolina Grąt; Arkadiusz Antczak; Joanna Ligocka; Wacław Hołówko; Karolina M. Wronka; Konrad Kobryń; Michał Skalski; Leszek Pączek; Marek Krawczyk

UNLABELLED The number of elderly patients undergoing liver transplantation (LT) is increasing worldwide. The aim of the study was to evaluate the impact of recipient age exceeding 60 years on early and long-term outcomes after LT. MATERIAL AND METHODS This study comprised data of 786 patients after primary LT performed at a single center between January 2005 and October 2012. Patients over and under 60 years of age were compared with respect to baseline characteristics and outcomes: postoperative mortality (90-day) and 5-year patient (PS) and graft (GS) survival. Associations between recipient age exceeding 60 years and LT results were assessed in multiple Cox regression models. RESULTS Recipients older than 60 years (n=107; 13.6%) were characterized by more frequent hepatitis C virus infections (p<0.001), malignancies (p<0.001), and cardiovascular comorbidities (p<0.001); less frequent primary sclerosing cholangitis (p=0.002) and Roux-en-Y hepaticojejunostomy (p<0.001); lower Model for End-stage Liver Disease (MELD; p=0.043); and increased donor age (p=0.012). Fiveyear PS of older and younger recipients was 72.7% and 80.6% (p=0.538), while the corresponding rates of GS were 70.3% and 77.5% (p=0.548), respectively. Recipient age exceeding 60 years was not significantly associated with postoperative mortality (p=0.215), PS (p=0.525) and GS (p=0.572) in multivariate analyses. The list of independent predictors comprised MELD (p<0.001) for postoperative mortality; malignancies (p=0.003) and MELD (p<0.001) for PS; and malignancies (p=0.003), MELD (p<0.001) and donor age (p=0.017) for GS. CONCLUSIONS Despite major differences between elderly and young patients, chronological age exceeding 60 years alone should not be considered as a contraindication for LT.


Scientific Reports | 2017

Limitations of predicting microvascular invasion in patients with hepatocellular cancer prior to liver transplantation

Michał Grąt; Jan Stypułkowski; Waldemar Patkowski; Emil Bik; Maciej Krasnodębski; Karolina M. Wronka; Zbigniew Lewandowski; Michał Wasilewicz; Karolina Grąt; Łukasz Masior; Joanna Ligocka; Marek Krawczyk

Microvascular invasion (MVI) is well known to negatively influence outcomes following surgical treatment of hepatocellular cancer (HCC) patients. The aim of this study was to evaluate the rationale for prediction of MVI before liver transplantation (LT). Data of 200 HCC patients after LT were subject to retrospective analysis. MVI was present in 57 patients (28.5%). Tumor number (p = 0.001) and size (p = 0.009), and alpha-fetoprotein (p = 0.049) were independent predictors of MVI used to create a prediction model, defined as: 0.293x(tumor number) + 0.283x(tumor size in cm) + 0.164xloge(alpha-fetoprotein in ng/ml) (c statistic  =  0.743). The established cut-off (≥2.24) was associated with sensitivity and specificity of 72%. MVI was not an independent risk factor for recurrence (p = 0.307), in contrast to tumor number (p = 0.047) and size (p < 0.001), alpha-fetoprotein (p < 0.001) and poor differentiation (p = 0.039). Recurrence-free survival at 5 years for patients without MVI was 85.9% as compared to 83.3% (p = 0.546) and 55.3% (p = 0.001) for patients with false negative and true positive prediction of MVI, respectively. The use of both morphological and biological tumor features enables effective pre-transplant prediction of high-risk MVI. Provided that these parameters are combined in selection of HCC patients for LT, pre-transplant identification of all patients with MVI does not appear necessary.


Scandinavian Journal of Gastroenterology | 2017

Does transient elastography correlate with liver fibrosis in patients with PSC? Laennec score-based analysis of explanted livers

Marcin Krawczyk; Joanna Ligocka; Mariusz Ligocki; Joanna Raszeja-Wyszomirska; Malgorzata Milkiewicz; Grzegorz Szparecki; Tomasz Ilczuk; Barbara Górnicka; K. Zieniewicz; Marek Krawczyk; Frank Lammert; Piotr Milkiewicz

Abstract Background and aims: Previous studies demonstrated a close correlation between transient elastography (TE) and liver histology in chronic liver diseases. Data on the accuracy of TE in primary sclerosing cholangitis (PSC) remains scarce. Here, we investigated the association between TE, serum marker of liver injury and histology of explanted livers in PSC patients. Methods: Thirty patients were prospectively recruited. TE (Fibroscan®) and blood sampling were performed during evaluation for liver transplantation (LT); the second blood sampling was performed on the day of LT. Fibrosis of explanted livers according to the seven-point Laennec staging system and liver collagen contents were measured. Results: TE correlated with Laennec stages of fibrosis (p = .001), collagen contents (p < .001) and with diameter of thickest septa (p = .034) in explanted livers. It also correlated with serum indices of liver injury, namely AST, bilirubin as well as FIB-4 and APRI scores (all p < .05). In a multivariate model, only liver fibrosis, according to either Laennec score (p = .035) or collagen contents (p = .005), was significantly associated with TE. Finally, patients with cirrhosis had increased liver stiffness (p = .002) and the TE cut-off of 13.7 kPa showed the best predictive value (AUC = .90, 95% CI: 0.80–1.00, p < .001) for detecting cirrhosis. Conclusions: TE correlates with liver fibrosis and markers of liver injury in patients with PSC. However, liver fibrosis seems to be the strongest predictor of liver stiffness assessed with TE. Hence, we postulate that TE is a reliable tool for non-invasive monitoring of PSC.


Polish Journal of Surgery | 2015

Liver resection for non-colorectal, non-endocrine liver metastasis.

Oskar Kornasiewicz; Joanna Ligocka; Marek Krawczyk

Liver metastases of non-colorectal non-endocrine origin (NCNELM) are rare indications for resection. Even in major liver surgery units, NCNELM constitute no more than 5% of all indications for resection. Such a small number is due to the fact that in the case of NCNELM, both primary and metastatic lesions are generally recognized in the advanced stages of the disease when not only metastases to the liver are present. Yet another important factor is the general belief that in the case of an advanced disease with the presence of liver lesions, surgical resection does not benefit patients. In terms of survival, despite differences in cancer biology, patients with NCNELM are often compared with the results of surgical treatment for colorectal liver metastases (CLM), for which resection has been now widely recognized as the treatment of choice. Additionally, in the case of CLM, chemotherapy treatment has significantly improved over the last several years, leading to an increase in potentially radical liver resections and reresections. This has led to a perspective where CLM are currently seen as a manifestation of the metastatic process with the possibility of effective surgical treatment. In Poland, the latest results of surgical treatment for CLM were presented by Dudek at al. with a 5-year survival of 47.6% (1). However resection of NCNELM has been only considered as a palliative treatment. On the other hand, the lack of effective chemotherapy for NCNELM leads to the conclusion that surgery is currently the only means of treatment which may lead to a potential cure. R E v I E w P A P E R S

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Marek Krawczyk

Medical University of Warsaw

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Waldemar Patkowski

Medical University of Warsaw

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Oskar Kornasiewicz

Medical University of Warsaw

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K. Zieniewicz

Medical University of Warsaw

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Michał Grąt

Medical University of Warsaw

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Piotr Milkiewicz

Medical University of Warsaw

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Karolina Grąt

Medical University of Warsaw

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Karolina M. Wronka

Medical University of Warsaw

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Maciej Krasnodębski

Medical University of Warsaw

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Michał Skalski

Medical University of Warsaw

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