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4. Clinical implications of serum autotoxin in regular follow up after pediatric living donor liver transplantation for biliary atresia

Author

1000010456957, Ueno, Takehisa, Takase, Koki, 1000010839369, Toyama, Chiyoshi, 1000000747082, Deguchi, Koichi, 1000040588381, Masahata, Kazunori, 1000040546909, Nomura, Motonari, 1000040791728, Watanabe, Miho, 1000020403074, Kamiyama, Masafumi, 1000010397698, Tazuke, Yuko, 1000080423169, Bessho, Kazuhiko, 1000030252670, Okuyama, Hiroomi, 1000010456957, Ueno, Takehisa, Takase, Koki, 1000010839369, Toyama, Chiyoshi, 1000000747082, Deguchi, Koichi, 1000040588381, Masahata, Kazunori, 1000040546909, Nomura, Motonari, 1000040791728, Watanabe, Miho, 1000020403074, Kamiyama, Masafumi, 1000010397698, Tazuke, Yuko, 1000080423169, Bessho, Kazuhiko, 1000030252670, and Okuyama, Hiroomi

Abstract

Background: : Pediatric patients sometimes develop graft fibrosis after living donor liver transplant (LDLT). Autotaxin is a recently developed serum marker for hepatic fibrosis. We studied the relationship between serum autotaxin levels and histological findings in patients after LDLT for biliary atresia (BA). Methods: Information on patients aged <19 years who received LDLT for BA and were followed for at least 1 year after LDLT was gathered. Autotaxin levels were compared with pathological fibrosis scores. Results: The study included 52 patients, of whom 4 patients had no fibrosis (F0), 36 patients had F1 fibrosis, and 12 patients had F2. The median serum autotaxin level was 0.89 mg/L. In patients with portal vein (PV) complications such as stenosis or thrombosis (n = 7), the mean autotoxin level was 1.25 mg/L compared with 0.95 mg/L in patients without PV complications (p = 0.004). Among patients without PV complications, the mean autotaxin level was 0.90, 0.88, and 1.18 mg/L in F0, F1, and F2 fibrosis, respectively. The mean autotaxin was higher in F2 fibrosis than in F0 or F1 fibrosis (p<0.05). Autotoxin had a high area under the curve (0.86) with the cut-off level of 0.897 mg/L. Conclusion: Serum autotaxin is a novel marker for liver fibrosis in patients after pediatric LDLT for BA. Type of study: : Study of Diagnostic Test. Level of evidence: : Level II.

Published
2022

10. Cancer's Achilles' Heel: Apoptosis and Necroptosis to the Rescue.

Author

Dasgupta, Atreyi, Nomura, Motonari, Shuck, Ryan, and Yustein, Jason

Subjects
*APOPTOSIS, *CANCER cells, *TUMOR suppressor genes, *ONCOGENES, *CANCER chemotherapy, *CELL death
Abstract

Apoptosis, and the more recently discovered necroptosis, are two avenues of programmed cell death. Cancer cells survive by evading these two programs, driven by oncogenes and tumor suppressor genes. While traditional therapy using small molecular inhibitors and chemotherapy are continuously being utilized, a new and exciting approach is actively underway by identifying and using synergistic relationship between driver and rescue genes in a cancer cell. Through these synthetic lethal relationships, we are gaining tremendous insights into tumor vulnerabilities and specific molecular avenues for induction of programmed cell death. In this review, we briefly discuss the two cell death processes and cite examples of such synergistic manipulations for therapeutic purposes. [ABSTRACT FROM AUTHOR]

Published
2017
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12. Abstract 4359: TRAIL and Noxa are selectively up-regulated in prostate cancer cells downstream of the RIG-I/MAVS signaling pathway by non-replicating Sendai virus particles.

Author

Hatano, Koji, primary, Nakai, Yasutomo, additional, Matsushima-Miyagi, Taeko, additional, Nomura, Motonari, additional, Nakata, Wataru, additional, Yoshida, Takahiro, additional, Sato, Mototaka, additional, Kawashima, Atsunari, additional, Nagahara, Akira, additional, Fujita, Kazutoshi, additional, Uemura, Motohide, additional, Takayama, Hitoshi, additional, Kaneda, Yasufumi, additional, and Nonomura, Norio, additional

Published
2013
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15. Serum Trough Concentration and Effects of Mycophenolate Mofetil Based on Pathologic Findings in Infants After Liver Transplantation

Author

Ueno, Takehisa, Kodama, Tasuku, Noguchi, Yuki, Deguchi, Koichi, Nomura, Motonari, Saka, Ryuta, Watanabe, Miho, Tazuke, Yuko, Bessho, Kazuhiko, Okuyama, Hiroomi, Ueno, Takehisa, Kodama, Tasuku, Noguchi, Yuki, Deguchi, Koichi, Nomura, Motonari, Saka, Ryuta, Watanabe, Miho, Tazuke, Yuko, Bessho, Kazuhiko, and Okuyama, Hiroomi

Abstract

Ueno T., Kodama T., Noguchi Y., et al. Serum Trough Concentration and Effects of Mycophenolate Mofetil Based on Pathologic Findings in Infants After Liver Transplantation. Transplantation Proceedings 52, 1855 (2020); https://doi.org/10.1016/j.transproceed.2020.01.160., Objectives: Mycophenolate mofetil (MMF) is mainly used in conjunction with calcineurin inhibitors as an additional immunosuppressive for renal sparing after liver transplantation. However, few reports about MMF use in infants after living donor liver transplantation (LDLT) are available. The purpose of this study was to examine the efficacy and safety of MMF in infants. Methods: This study enrolled infants younger than 1 year of age who received LDLT at our institution. Patients received oral MMF twice daily. The initial dose was 40 to 50 mg/kg/d, which was increased to a target mycophenolic acid (MPA) trough level of 2 mg/L. Body weight, height, MMF dose, MPA trough level, acute cellular rejection (ACR) episodes, pathologic findings, and adverse effects were analyzed. Allograft fibrosis was graded using the Meta-analysis of Histological Data in Viral Hepatitis score. Results: Patients received MMF for refractory ACR (n = 2), fulminant hepatitis (n = 2), and pre-existing antibodies (n = 1). Original diseases were biliary atresia (n = 3) and fulminant hepatitis (n = 2). Mean age at transplant was 8 months (range 3-10 months). The last available mean trough level was 2.7 mg/L. The mean dose was 66 mg/kg/d or 1429 mg/m2/d at the time of the last available through level. The regression line for MMF dose and MPA trough level was y = 1.8 × 10-3x. The correlation coefficient was 0.65. All allografts showed F1 to F2 fibrosis. Two patients discontinued MMF because of infection and bone marrow suppression, respectively. Two patients converted to everolimus. One patient continued on MMF. Conclusions: After LDLT, infants require a higher MMF dose than older patients based on trough levels, but allograft fibrosis can progress.

16. Long-Term Outcome After Tacrolimus-Related Neurotoxicity in Pediatric Living Donor Liver Transplantation

Author

Ueno, Takehisa, Toyama, Chiyoshi, Deguchi, Koichi, Masahata, Kazunori, Nomura, Motonari, Watanabe, Miho, Kamiyama, Masafumi, Tazuke, Yuko, Bessho, Kazuhiko, Okuyama, Hiroomi, Ueno, Takehisa, Toyama, Chiyoshi, Deguchi, Koichi, Masahata, Kazunori, Nomura, Motonari, Watanabe, Miho, Kamiyama, Masafumi, Tazuke, Yuko, Bessho, Kazuhiko, and Okuyama, Hiroomi

Abstract

Ueno T., Toyama C., Deguchi K., et al. Long-Term Outcome After Tacrolimus-Related Neurotoxicity in Pediatric Living Donor Liver Transplantation. Transplantation Proceedings 54, 468 (2022); https://doi.org/10.1016/j.transproceed.2021.12.036., Background: Tacrolimus-related neurotoxicity is a serious complication. Posterior reversible encephalopathy syndrome, which is severe neurotoxicity after pediatric living donor liver transplantation (LDLT), is a medication-induced complication related to calcineurin inhibitors. The purpose of this study was to evaluate the long-term outcome of tacrolimus-related neurotoxicity after pediatric LDLT. Methods: Pediatric patients who underwent LDLT between 2007 and 2020 at our institution and developed neurologic symptoms with tacrolimus were included in the study. Tacrolimus-related encephalopathy was defined as encephalopathy that resolved after tacrolimus was discontinued. All patients received tacrolimus and a steroid for immunosuppression starting just after LDLT. Results: During the study period, 128 patients underwent LDLT. All patients received tacrolimus and a steroid. Six patients (5%) developed tacrolimus-related encephalopathy. The median age at transplant was 1.6 years. The original diseases were biliary atresia (n = 5) and progressive familial intrahepatic cholangiopathy type 2 (n = 1). Patients developed encephalopathy at a median of 9 days after LDLT. All patients recovered with conversion to cyclosporine. Posterior reversible encephalopathy syndrome was confirmed by magnetic resonance imaging in 3 patients. The mean tacrolimus level at encephalopathy was 11 ng/dL (range, 5.6-14.6 ng/dL). White blood cell count elevation was observed in all patients. One patient died of pancreatitis. Surviving patients (n = 5) were followed for a median of 9 years. All patients resumed tacrolimus a median of 8 months from onset. No neurologic complications were observed after resuming tacrolimus. Conclusion: We observed tacrolimus-induced encephalopathy in 5% of patients after pediatric LDLT. Patients can resume tacrolimus safely without further neurologic symptoms.

17. Early Use of Everolimus as a Third Immunosuppressive Agent for Intestinal Transplantation: A Report of 2 Cases

Author

Ueno, Takehisa, Toyama, Chiyoshi, Deguchi, Koichi, Masahata, Kazunori, Nomura, Motonari, Watanabe, Miho, Kamiyama, Masafumi, Tazuke, Yuko, Bessho, Kazuhiko, Okuyama, Hiroomi, Ueno, Takehisa, Toyama, Chiyoshi, Deguchi, Koichi, Masahata, Kazunori, Nomura, Motonari, Watanabe, Miho, Kamiyama, Masafumi, Tazuke, Yuko, Bessho, Kazuhiko, and Okuyama, Hiroomi

Abstract

Ueno T., Toyama C., Deguchi K., et al. Early Use of Everolimus as a Third Immunosuppressive Agent for Intestinal Transplantation: A Report of 2 Cases. Transplantation Proceedings 54, 472 (2022); https://doi.org/10.1016/j.transproceed.2022.01.010., Background: In patients with intestinal transplantation (ITx), renal function is easily impaired because of long-term parenteral nutrition and side effects of tacrolimus. Everolimus was used in patients with renal insufficiency in our study. Methods: We administered everolimus as a third immunosuppressive agent in addition to tacrolimus and steroids for renal sparing in patients who received ITx. We assessed everolimus levels, complications, and renal function. Results: Two patients received everolimus after ITx. Patient 1 was a 13-year-old boy who underwent ITx for an allied disorder of Hirschsprung's disease. After induction therapy with rabbit antithymocyte globulin, maintenance therapy consisted of tacrolimus and steroids. Everolimus was introduced 3 months after ITx for renal sparing. Seven months later, the patient required partial intestinal graft resection owing to bowel obstruction. Everolimus was suspended for only 2 weeks. Four years after ITx, the trough level of tacrolimus was maintained at 3 to 5 ng/mL. The trough level of everolimus was maintained at 3 to 5 ng/mL. Patient 2 was a 32-year-old man who underwent deceased ITx for short gut syndrome. Induction and maintenance immunosuppression was the same as for patient 1. Everolimus was introduced 1 month after surgery. Two years after ITx, trough levels of tacrolimus and everolimus were the same as in patient 1. No rejection was observed in either patient, and renal function was well maintained. We observed no side effects caused by everolimus. Conclusions: Everolimus could be used safely and effectively after ITx. Early use of everolimus after ITx did not affect wound healing.

18. Long-Term Outcome of Portal Vein Stenting After Pediatric Living Donor Liver Transplantation

Author

Ueno, Takehisa, Toyama, Chiyoshi, Deguchi, Koichi, Masahata, Kazunori, Nomura, Motonari, Watanabe, Miho, Kamiyama, Masafumi, Tazuke, Yuko, Bessho, Kazuhiko, Okuyama, Hiroomi, Ueno, Takehisa, Toyama, Chiyoshi, Deguchi, Koichi, Masahata, Kazunori, Nomura, Motonari, Watanabe, Miho, Kamiyama, Masafumi, Tazuke, Yuko, Bessho, Kazuhiko, and Okuyama, Hiroomi

Abstract

Ueno T., Toyama C., Deguchi K., et al. Long-Term Outcome of Portal Vein Stenting After Pediatric Living Donor Liver Transplantation. Transplantation Proceedings 54, 454 (2022); https://doi.org/10.1016/j.transproceed.2022.01.008., Background: Portal vein (PV) stenosis is sometimes seen in pediatric living donor liver transplantation (LDLT). PV stents have been attempted in adults with persistent stenosis. However, long-term usefulness of PV stenting is unknown because stents do not expand with growth. We investigated the effect and long-term outcome of PV stenting for stenosis after pediatric LDLT. Methods: We included patients aged <18 years who underwent LDLT from 1998 to 2020 and who underwent PV stenting for stenosis. We assessed age at procedure, stent complications, and long-term outcomes. Results: Five patients underwent PV stent placement. The median age at LDLT was 10 years (range, 0.8-18.1 years). The median interval between LDLT and stent placement was 25 months. The median age at stent placement was 16 years (range, 3-20 years). The median body weight was 38 kg (range, 13-63 kg). The median stent diameter was 8 mm. The median observation period after stent placement was 8 years. On average, body weight increased 1.6 times. One complication associated with stent placement was PV thrombosis, which resulted in stent failure, but we observed no portal hypertension. In the other 4 patients, the stent has remained functioning, and there was no clinical evidence of portal hypertension. Conclusions: PV stents are effective for intractable PV stenosis in children. PV stents were successfully placed in children as young as 3 years old and weighing 13 kg. Our data suggests that a stent placed in young children does not cause portal hypertension as patients grow.

19. Beta-D-Glucan Levels With Use of an Anti-adhesion Barrier Film in Pediatric Living Donor Liver Transplantation

Author

Ueno, Takehisa, Kodama, Tasuku, Noguchi, Yuki, Deguchi, Koichi, Nomura, Motonari, Saka, Ryuta, Watanabe, Miho, Tazuke, Yuko, Bessho, Kazuhiko, Okuyama, Hiroomi, Ueno, Takehisa, Kodama, Tasuku, Noguchi, Yuki, Deguchi, Koichi, Nomura, Motonari, Saka, Ryuta, Watanabe, Miho, Tazuke, Yuko, Bessho, Kazuhiko, and Okuyama, Hiroomi

Abstract

Ueno T., Kodama T., Noguchi Y., et al. Beta-D-Glucan Levels With Use of an Anti-adhesion Barrier Film in Pediatric Living Donor Liver Transplantation. Transplantation Proceedings 52, 1818 (2020); https://doi.org/10.1016/j.transproceed.2020.02.147., Introduction: Serum beta-D-glucan (BDG) levels may increase with anti-adhesion barrier film (ABF) use during pediatric living donor liver transplantation (LDLT). It may affect detection of fungal infections after LDLT. We evaluate BDG levels after pediatric LDLT. Methods: Pediatric patients who received an ABF during LDLT were included. Patients who may have had fungal infections prior to LDLT were excluded. One sheet of ABF was placed in the peritoneum during abdominal closure. Serum BDG levels before transplantation and on postoperative days (PODs) 1, 4, 7, 14, 21, and 28 and peritoneal fluid BDG levels on PODs 1 and 7 were measured. Results: Sixteen patients received an ABF during LDLT. Median age at transplant was 1.9 years (range, 6-11 years). Median body weight was 12.6 kg (range, 6.8-39 kg). Indications for LDLT were biliary atresia (n = 10) and other (n = 5). Prior to transplantation, the mean serum BDG level was 3.8 pg/mL. Mean Serum BDG levels were 18.1, 38.3, 5.3, 3.8, 3.3, and 3.3 pg/mL on PODs 1, 4, 7, 14, 21, and 28, respectively. Mean peritoneal fluid BDG levels were 485.9 and 240.4 pg/mL on PODs 1 and 7, respectively. No clinical fungal infections were observed. Conclusions: BDG levels were high in serum and peritoneal fluid after pediatric LDLT. Serum BDG levels normalized after POD 7. Careful interpretation of BDG levels until POD 7 is needed when an ABF has been used.

20. Impact of Monosegment Graft Use for Infants in Pediatric Living Donor Liver Transplantation

Author

Ueno, Takehisa, Toyama, Chiyoshi, Deguchi, Koichi, Masahata, Kazunori, Nomura, Motonari, Watanabe, Miho, Kamiyama, Masafumi, Tazuke, Yuko, Bessho, Kazuhiko, Okuyama, Hiroomi, Ueno, Takehisa, Toyama, Chiyoshi, Deguchi, Koichi, Masahata, Kazunori, Nomura, Motonari, Watanabe, Miho, Kamiyama, Masafumi, Tazuke, Yuko, Bessho, Kazuhiko, and Okuyama, Hiroomi

Abstract

Ueno T., Toyama C., Deguchi K., et al. Impact of Monosegment Graft Use for Infants in Pediatric Living Donor Liver Transplantation. Transplantation Proceedings 54, 391 (2022); https://doi.org/10.1016/j.transproceed.2021.12.034., Background: Left lateral segment grafts are generally used for very young pediatric patients undergoing living donor liver transplantation (LDLT). Recently, graft reduction techniques were developed for LDLT. Monosegment grafting has been used in newborns. The aim of this study was to determine the usefulness of monosegment grafting for infants. Methods: Recipients <2 years of age who underwent LDLT with a monosegment graft between 2010 and 2020 were gathered. Parents comprised all LDLT donors. A segment 2 monosegment graft was resected as a graft from the donor. Standard liver volume (SLV) was estimated using Urata's equation. Graft type, graft weight (GW), and native liver weight were assessed. Results: Eight patients were included in the study. Original diseases consisted of biliary atresia (n = 6) and fulminant hepatitis (n = 2). Final graft type included monosegment (n = 5) and reduced monosegment (n = 3). Median final GW/body weight after reduction was 3% (range, 2%-3.4%). Median native liver weight/SLV was 134% except in patients with fulminant hepatitis. Median pre-reduction graft volume (GV)/estimated GV was 113% (range, 60%-208%). Median pre-reduction GV/SLV of monosegment grafts that required reduction (n = 3) was 109% (range, 106%-121%). Median final reduced graft GV/SLV was 80% (range, 74%-91%). Complications due to large-for-size grafts were not observed. One case of bile leakage due to graft reduction occurred as a complication. Grafts were functioning well with the exception of one graft loss due to antibody-mediated rejection. Conclusion: Estimated GV in infants varies widely. Monosegment grafting can be useful for infants as well as newborns.

21. One Year of Preemptive Valganciclovir Administration in Children After Liver Transplantation

Author

Ueno, Takehisa, Kodama, Tasuku, Noguchi, Yuki, Deguchi, Koichi, Nomura, Motonari, Saka, Ryuta, Watanabe, Miho, Tazuke, Yuko, Bessho, Kazuhiko, Okuyama, Hiroomi, Ueno, Takehisa, Kodama, Tasuku, Noguchi, Yuki, Deguchi, Koichi, Nomura, Motonari, Saka, Ryuta, Watanabe, Miho, Tazuke, Yuko, Bessho, Kazuhiko, and Okuyama, Hiroomi

Abstract

Ueno T., Kodama T., Noguchi Y., et al. One Year of Preemptive Valganciclovir Administration in Children After Liver Transplantation. Transplantation Proceedings 52, 1852 (2020); https://doi.org/10.1016/j.transproceed.2020.01.163., Objectives: Valganciclovir (VGCV) is used as prophylaxis against cytomegalovirus (CMV) infection after pediatric living donor liver transplantation (LDLT). The purpose of this study was to examine the efficacy of 1 year of preemptive VGCV administration compared with a shorter administration after pediatric LDLT. Methods: VGCV was administered to 56 children who underwent LDLT. CMV and Epstein-Barr virus (EBV) antibody status, pp65 antigenemia, and other laboratory data were assessed at 1 year after LDLT. Patients were divided into the 1-year group (n = 32) (patients who had 1 year of VGCV administration) and the <1-year group (n = 24) (patients who had less than 1 year of VGCV administration). Results: Study participants consisted of 34 females and 22 males, with a mean age of 4.2 years at transplant. Regarding pretransplant donor (D)/recipient (R) CMV antibody status, 13 were D positive (+)/R negative (-), 27 were D+/R+, 8 were D-/R+, and 8 were D-/R-. For EBV, 22 were D+/R+, 32 were D+/R-, and 2 were D-/R-. In the 1-year group, only 2 patients (6.5%) developed CMV infection, whereas 8 patients (33.3%) developed CMV infection in the <1-year group. The CMV pp65 antigenemia assay was positive in 2 patients. CMV IgM was positive in 7 patients. One year of preemptive VGCV administration was associated with a lower incidence of CMV infection (P = .008), but not EBV infection. No adverse effects were observed. Conclusions: One year of preemptive VGCV administration after LDLT is safe and suppresses CMV infection. It was useful after pediatric LDLT.

22. Safety and Efficacy of Everolimus Rescue Treatment After Pediatric Living Donor Liver Transplantation

Author

Ueno, Takehisa, Kodama, Tasuku, Noguchi, Yuki, Deguchi, Koichi, Nomura, Motonari, Saka, Ryuta, Watanabe, Miho, Tazuke, Yuko, Bessho, Kazuhiko, Okuyama, Hiroomi, Ueno, Takehisa, Kodama, Tasuku, Noguchi, Yuki, Deguchi, Koichi, Nomura, Motonari, Saka, Ryuta, Watanabe, Miho, Tazuke, Yuko, Bessho, Kazuhiko, and Okuyama, Hiroomi

Abstract

Ueno T., Kodama T., Noguchi Y., et al. Safety and Efficacy of Everolimus Rescue Treatment After Pediatric Living Donor Liver Transplantation. Transplantation Proceedings 52, 1829 (2020); https://doi.org/10.1016/j.transproceed.2020.01.159., Purpose: Everolimus (EVR) is a derivative of sirolimus with a similar mechanism of action. The safety and efficacy of EVR after pediatric living donor liver transplantation (LDLT) are currently unknown. The purpose of this study was to examine the safety and efficacy of EVR as rescue therapy after pediatric LDLT. Methods: This study included patients younger than 19 years of age who received EVR after LDLT at our institution. EVR was administered as rescue treatment in addition to tacrolimus. In 21 patients, EVR dose, trough level, outcomes, and adverse effects were assessed. Results: Original diseases of patients consisted of biliary atresia (n = 11), Alagille syndrome (n = 3), fulminant hepatitis (n = 3), hepatoblastoma (n = 2), and other (n = 2). Mean age at transplant was 2.0 years (range 0.6-6.2 years). Mean age at initial EVR administration was 8.0 years (range 0.9-18.9 years). Indications for EVR use were graft fibrosis (n = 8), refractory acute cellular rejection (n = 5), renal sparing (n = 4), hepatoblastoma (n = 2), and chronic rejection (CR) (n = 2). Mean duration of administration was 17.1 months (range 2.1-60.4 months). Mean dose was 0.5 mg/m2 twice daily. Mean EVR trough level was 2.5 ng/mL (range 1.5-5.0 ng/mL). Liver function improved and fibrosis did not progress in all patients with CR. However, 14 patients (67%) experienced adverse effects that required EVR dose reduction or discontinuation. Conclusion: EVR is tolerable for pediatric patients after LDLT with dose adjustment. EVR had a certain effect to relieve progression on CR. Further follow-up is required.

23. Effect of microscopy-assisted portoenterostomy (MAPE) for biliary atresia

Author

Ueno, Takehisa, Kodama, Tasuku, Noguchi, Yuki, Nomura, Motonari, Saka, Ryuta, Takama, Yuichi, Tazuke, Yuko, Bessho, Kazuhiko, Okuyama, Hiroomi, Ueno, Takehisa, Kodama, Tasuku, Noguchi, Yuki, Nomura, Motonari, Saka, Ryuta, Takama, Yuichi, Tazuke, Yuko, Bessho, Kazuhiko, and Okuyama, Hiroomi

Abstract

This version of the article has been accepted for publication, after peer review (when applicable) and is subject to Springer Nature’s AM terms of use, but is not the Version of Record and does not reflect post-acceptance improvements, or any corrections. The Version of Record is available online at: https://doi.org/10.1007/s00383-020-04794-x., Purpose: Portoenterostomy (PE) is the standard treatment for biliary atresia (BA). However, micro-bile ducts are difficult to identify with surgical loupes and dissect systematically. We report the effects of our attempts to dissect hilar tissue using a surgical microscope. Methods: Microscopy-assisted portoenterostomy (MAPE) was initiated in 2014. Patients born between 2000 and 2013 who underwent PE until day 70 without a surgical microscope for BA were gathered as historical control. MAPE in re-do PE cases (Re-MAPE) was evaluated in the same manner. Results: Ten patients underwent MAPE for BA during the study period. 17 patients in the conventional PE group were gathered. In the MAPE group, the jaundice clearance rate was 80%, compared with 53% in the conventional PE group. Re-MAPE was performed in four patients, who had a jaundice clearance rate of 75%, essentially identical to the rate with initial MAPE. At age 4 years, the native liver survival rate was 58% in the MAPE group and 38% in the conventional PE group. The native liver survival rate in the Re-MAPE group was 75%. Conclusion: MAPE is useful for sharing the surgical field during open PE in patients with BA. It may improve the rate of jaundice clearance.

24. Balloon dilatation for congenital esophageal stenosis associated with esophageal atresia

Author

Deguchi, Koichi, Kamiyama, Masafumi, Masahata, Kazunori, Nomura, Motonari, Watanabe, Miho, Ueno, Takehisa, Tazuke, Yuko, Okuyama, Hiroomi, Deguchi, Koichi, Kamiyama, Masafumi, Masahata, Kazunori, Nomura, Motonari, Watanabe, Miho, Ueno, Takehisa, Tazuke, Yuko, and Okuyama, Hiroomi

Abstract

The version of record of this article, first published in Pediatric Surgery International, is available online at Publisher’s website: https://doi.org/10.1007/s00383-024-05652-w., Purpose: Congenital esophageal stenosis (CES) associated with esophageal atresia (EA) is rare, and no standard treatment has been established. We reviewed cases of EA-associated CES to assess the clinical characteristics and treatment outcomes, especially the feasibility of endoscopic dilatation. Methods: We retrospectively examined patients with EA-associated CES. We also compared treatment outcomes of EA-associated CES with those of EA patients without CES who developed postoperative anastomotic stricture. Results: Among 44 patients with EA, ten had CES (23%). Postoperative complications were not significantly different between EA patients with CES and those without CES but with anastomotic stricture. All CES patients underwent balloon dilatation as initial treatment. Eight of nine patients (89%) were successfully treated by dilatation only, and one patient underwent surgical resection. The median number of balloon dilatations for CES was five (2–17), which was higher than that for anastomotic stricture in patients without CES (p = 0.012). Esophageal perforation occurred in five patients with CES (5/9, 56%) after dilatation, but all perforations were successfully managed conservatively with an uneventful post-dilatation course. Conclusions: Twenty-three percent of patients with EA had CES. Although balloon dilatation for EA-associated CES required multiple treatments and carried a risk of perforation, balloon dilatation showed an 89% success rate and all perforations could be managed conservatively.

25. Plasma Concentration of Antifungal Agent Micafungin for Pediatric Living Donor Liver Transplantation

Author

Ueno, Takehisa, Takase, Koki, Deguchi, Koichi, Nomura, Motonari, Watanabe, Miho, Kamiyama, Masafumi, Tazuke, Yuko, Kimura, Takeshi, Okuyama, Hiroomi, Ueno, Takehisa, Takase, Koki, Deguchi, Koichi, Nomura, Motonari, Watanabe, Miho, Kamiyama, Masafumi, Tazuke, Yuko, Kimura, Takeshi, and Okuyama, Hiroomi

Abstract

Ueno T., Takase K., Deguchi K., et al. Plasma Concentration of Antifungal Agent Micafungin for Pediatric Living Donor Liver Transplantation. Transplantation Proceedings 56, 602 (2024); https://doi.org/10.1016/j.transproceed.2024.01.020., Background: Pediatric living-donor liver transplantation (LDLT) candidates often receive long-term antibiotic treatment. Micafungin has been used as an antifungal agent after LDLT, but the adequate dose after pediatric LDLT was unknown. Here, we report micafungin blood concentrations after pediatric LDLT and discuss its safety and adequate dosing. Methods: Pediatric patients with data on micafungin concentrations after LDLT were identified. Those with surgical complications were excluded. All patients received standard tacrolimus-based immunosuppression. A micafungin dose of 1 mg/kg was administered once daily for 10 days starting on postoperative day (POD) 1. The trough and peak micafungin blood concentrations were evaluated on PODs 1, 4, 7, and 10. Beta D glucan levels and liver function tests were assessed to determine micafungin effectiveness and safety. Results: Ten patients were enrolled, with a median age of 1.2 years. The median graft vs body weight ratio was 2.7%. The primary diseases were biliary atresia (n = 7), Alagille syndrome (n = 2), and progressive familial intrahepatic cholestasis type 2 (n = 1). Mean peak micafungin levels were 4.47, 6.27, 5.47, and 5.47 µg/mL on PODs 1, 4, 7, and 10, respectively. Mean trough levels were 2.03, 1.88, and 2.66 µg/mL on PODs 4, 7, and 10, respectively. The micafungin half-lives were 13.7, 14.7, and 14.0 hours on PODs 4, 7, and 10, respectively. Beta D glucan levels were 4.4 pg/mL and 3.7 pg/mL before and after transplantation, respectively, indicating no significant difference (P = .3). No clinical fungal infections were observed. Conclusion: Micafungin administration is safe and effective after pediatric LDLT.

26. Impact of Total Parenteral Nutrition on Preoperative Management of Pediatric Living-Donor Liver Transplantation for Biliary Atresia Under 2 Years Old

Author

Ueno, Takehisa, Takase, Koki, Deguchi, Koichi, Nomura, Motonari, Watanabe, Miho, Kamiyama, Masafumi, Tazuke, Yuko, Kimura, Takeshi, Okuyama, Hiroomi, Ueno, Takehisa, Takase, Koki, Deguchi, Koichi, Nomura, Motonari, Watanabe, Miho, Kamiyama, Masafumi, Tazuke, Yuko, Kimura, Takeshi, and Okuyama, Hiroomi

Abstract

Ueno T., Takase K., Deguchi K., et al. Impact of Total Parenteral Nutrition on Preoperative Management of Pediatric Living-Donor Liver Transplantation for Biliary Atresia Under 2 Years Old. Transplantation Proceedings 56, 605 (2024); https://doi.org/10.1016/j.transproceed.2024.01.017., Background: Liver failure and gastrointestinal bleeding occur in the end-stage of biliary atresia (BA). Living-donor liver transplantation (LDLT) is a standard treatment in Japan. Our program actively provides pre-transplant total parenteral nutrition (TPN) for such patients, and here we report its efficiency and safety. Methods: Patients with BA for whom LDLT was indicated were identified. Those with a long-term external central venous catheter and TPN, longer than 4 weeks before LDLT, were analyzed. Ascites was controlled with diuretics. TPN indications, efficacy, and complications were assessed along with patient growth, biochemical markers, and gastrointestinal bleeding. Results: Fourteen patients were included in the study, of whom 8 were girls and 6 were boys. The median age at LDLT was 0.9 years. Body weight (BW) at TPN initiation averaged 6799 g, and the median serum total bilirubin was 9.5 mg per dL. The median catheterization duration was 54 days, and 1 patient received home TPN. Indications for TPN were gastrointestinal bleeding and/or massive esophageal varices in 4 patients and poor nutritional status in 10 patients. No complications were observed except for 1 catheter infection and 1 catheter occlusion. The median final body weight before LDLT was 7906 g. The mean rate of BW gain was significantly higher after TPN than before (149 vs 32 g/wk, respectively, P = .0002). Mean prothrombin time and levels of albumin, cholinesterase, and total bilirubin were not significantly different at the start and end of TPN. Conclusions: Pre-transplant TPN was safe and effective for patients with end-stage BA.

27. Long-Term Outcome After Tacrolimus-Related Neurotoxicity in Pediatric Living Donor Liver Transplantation

Author

Ueno, Takehisa, Toyama, Chiyoshi, Deguchi, Koichi, Masahata, Kazunori, Nomura, Motonari, Watanabe, Miho, Kamiyama, Masafumi, Tazuke, Yuko, Bessho, Kazuhiko, Okuyama, Hiroomi, Ueno, Takehisa, Toyama, Chiyoshi, Deguchi, Koichi, Masahata, Kazunori, Nomura, Motonari, Watanabe, Miho, Kamiyama, Masafumi, Tazuke, Yuko, Bessho, Kazuhiko, and Okuyama, Hiroomi

Abstract

Ueno T., Toyama C., Deguchi K., et al. Long-Term Outcome After Tacrolimus-Related Neurotoxicity in Pediatric Living Donor Liver Transplantation. Transplantation Proceedings 54, 468 (2022); https://doi.org/10.1016/j.transproceed.2021.12.036., Background: Tacrolimus-related neurotoxicity is a serious complication. Posterior reversible encephalopathy syndrome, which is severe neurotoxicity after pediatric living donor liver transplantation (LDLT), is a medication-induced complication related to calcineurin inhibitors. The purpose of this study was to evaluate the long-term outcome of tacrolimus-related neurotoxicity after pediatric LDLT. Methods: Pediatric patients who underwent LDLT between 2007 and 2020 at our institution and developed neurologic symptoms with tacrolimus were included in the study. Tacrolimus-related encephalopathy was defined as encephalopathy that resolved after tacrolimus was discontinued. All patients received tacrolimus and a steroid for immunosuppression starting just after LDLT. Results: During the study period, 128 patients underwent LDLT. All patients received tacrolimus and a steroid. Six patients (5%) developed tacrolimus-related encephalopathy. The median age at transplant was 1.6 years. The original diseases were biliary atresia (n = 5) and progressive familial intrahepatic cholangiopathy type 2 (n = 1). Patients developed encephalopathy at a median of 9 days after LDLT. All patients recovered with conversion to cyclosporine. Posterior reversible encephalopathy syndrome was confirmed by magnetic resonance imaging in 3 patients. The mean tacrolimus level at encephalopathy was 11 ng/dL (range, 5.6-14.6 ng/dL). White blood cell count elevation was observed in all patients. One patient died of pancreatitis. Surviving patients (n = 5) were followed for a median of 9 years. All patients resumed tacrolimus a median of 8 months from onset. No neurologic complications were observed after resuming tacrolimus. Conclusion: We observed tacrolimus-induced encephalopathy in 5% of patients after pediatric LDLT. Patients can resume tacrolimus safely without further neurologic symptoms.

28. Safety and Efficacy of Everolimus Rescue Treatment After Pediatric Living Donor Liver Transplantation

Author

Ueno, Takehisa, Kodama, Tasuku, Noguchi, Yuki, Deguchi, Koichi, Nomura, Motonari, Saka, Ryuta, Watanabe, Miho, Tazuke, Yuko, Bessho, Kazuhiko, Okuyama, Hiroomi, Ueno, Takehisa, Kodama, Tasuku, Noguchi, Yuki, Deguchi, Koichi, Nomura, Motonari, Saka, Ryuta, Watanabe, Miho, Tazuke, Yuko, Bessho, Kazuhiko, and Okuyama, Hiroomi

Abstract

Ueno T., Kodama T., Noguchi Y., et al. Safety and Efficacy of Everolimus Rescue Treatment After Pediatric Living Donor Liver Transplantation. Transplantation Proceedings 52, 1829 (2020); https://doi.org/10.1016/j.transproceed.2020.01.159., Purpose: Everolimus (EVR) is a derivative of sirolimus with a similar mechanism of action. The safety and efficacy of EVR after pediatric living donor liver transplantation (LDLT) are currently unknown. The purpose of this study was to examine the safety and efficacy of EVR as rescue therapy after pediatric LDLT. Methods: This study included patients younger than 19 years of age who received EVR after LDLT at our institution. EVR was administered as rescue treatment in addition to tacrolimus. In 21 patients, EVR dose, trough level, outcomes, and adverse effects were assessed. Results: Original diseases of patients consisted of biliary atresia (n = 11), Alagille syndrome (n = 3), fulminant hepatitis (n = 3), hepatoblastoma (n = 2), and other (n = 2). Mean age at transplant was 2.0 years (range 0.6-6.2 years). Mean age at initial EVR administration was 8.0 years (range 0.9-18.9 years). Indications for EVR use were graft fibrosis (n = 8), refractory acute cellular rejection (n = 5), renal sparing (n = 4), hepatoblastoma (n = 2), and chronic rejection (CR) (n = 2). Mean duration of administration was 17.1 months (range 2.1-60.4 months). Mean dose was 0.5 mg/m2 twice daily. Mean EVR trough level was 2.5 ng/mL (range 1.5-5.0 ng/mL). Liver function improved and fibrosis did not progress in all patients with CR. However, 14 patients (67%) experienced adverse effects that required EVR dose reduction or discontinuation. Conclusion: EVR is tolerable for pediatric patients after LDLT with dose adjustment. EVR had a certain effect to relieve progression on CR. Further follow-up is required.

29. One Year of Preemptive Valganciclovir Administration in Children After Liver Transplantation

Author

Ueno, Takehisa, Kodama, Tasuku, Noguchi, Yuki, Deguchi, Koichi, Nomura, Motonari, Saka, Ryuta, Watanabe, Miho, Tazuke, Yuko, Bessho, Kazuhiko, Okuyama, Hiroomi, Ueno, Takehisa, Kodama, Tasuku, Noguchi, Yuki, Deguchi, Koichi, Nomura, Motonari, Saka, Ryuta, Watanabe, Miho, Tazuke, Yuko, Bessho, Kazuhiko, and Okuyama, Hiroomi

Abstract

Ueno T., Kodama T., Noguchi Y., et al. One Year of Preemptive Valganciclovir Administration in Children After Liver Transplantation. Transplantation Proceedings 52, 1852 (2020); https://doi.org/10.1016/j.transproceed.2020.01.163., Objectives: Valganciclovir (VGCV) is used as prophylaxis against cytomegalovirus (CMV) infection after pediatric living donor liver transplantation (LDLT). The purpose of this study was to examine the efficacy of 1 year of preemptive VGCV administration compared with a shorter administration after pediatric LDLT. Methods: VGCV was administered to 56 children who underwent LDLT. CMV and Epstein-Barr virus (EBV) antibody status, pp65 antigenemia, and other laboratory data were assessed at 1 year after LDLT. Patients were divided into the 1-year group (n = 32) (patients who had 1 year of VGCV administration) and the <1-year group (n = 24) (patients who had less than 1 year of VGCV administration). Results: Study participants consisted of 34 females and 22 males, with a mean age of 4.2 years at transplant. Regarding pretransplant donor (D)/recipient (R) CMV antibody status, 13 were D positive (+)/R negative (-), 27 were D+/R+, 8 were D-/R+, and 8 were D-/R-. For EBV, 22 were D+/R+, 32 were D+/R-, and 2 were D-/R-. In the 1-year group, only 2 patients (6.5%) developed CMV infection, whereas 8 patients (33.3%) developed CMV infection in the <1-year group. The CMV pp65 antigenemia assay was positive in 2 patients. CMV IgM was positive in 7 patients. One year of preemptive VGCV administration was associated with a lower incidence of CMV infection (P = .008), but not EBV infection. No adverse effects were observed. Conclusions: One year of preemptive VGCV administration after LDLT is safe and suppresses CMV infection. It was useful after pediatric LDLT.

30. Serum Mac-2-binding protein (M2BPGi) as a marker of chronological liver fibrosis in biliary atresia patients with cirrhosis

Author

Ueno, Takehisa, Kodama, Tasuku, Noguchi, Yuki, Nomura, Motonari, Saka, Ryuta, Takama, Yuichi, Tazuke, Yuko, Bessho, Kazuhiko, Okuyama, Hiroomi, Ueno, Takehisa, Kodama, Tasuku, Noguchi, Yuki, Nomura, Motonari, Saka, Ryuta, Takama, Yuichi, Tazuke, Yuko, Bessho, Kazuhiko, and Okuyama, Hiroomi

Abstract

This version of the article has been accepted for publication, after peer review (when applicable) and is subject to Springer Nature’s AM terms of use, but is not the Version of Record and does not reflect post-acceptance improvements, or any corrections. The Version of Record is available online at: https://doi.org/10.1007/s00383-019-04535-9, Purpose: Biliary atresia (BA) is characterized by progressive liver fibrosis, but it is difficult to assess the progression after the patient develops cirrhosis. Mac-2-binding protein glycosylation isomer (M2BPGi) is a new marker for hepatic fibrosis. We examined the chronological changes in M2BPGi levels in BA patients with cirrhosis. Methods: Patients with cirrhosis were selected from among pediatric BA patients who had their native livers. Serum M2BPGi levels and Child–Pugh classification were evaluated. A total of 11 pediatric BA patients with cirrhosis were recruited. Results: Initial M2BPGi level after diagnosis of liver cirrhosis based on liver biopsy was on average 3.4, and the most recent M2BPGi level under observation was on average 4.3. The follow-up period from the initial M2BPGi measurement averaged 22.6 months. The ratio of the initial and most recent values (M2BPGi ratio) was on average 1.3 (0.5–2.4). Three cases with improved fibrosis (M2BPGi ratio < 1.0) remained in Child A, as did six cases (1.0 ≤ M2BPGi ratio < 2.0), but two cases with marked fibrosis progression (2.0 ≤ M2BPGi ratio) advanced to decompensated cirrhosis Child B. Conclusion: M2BPGi is useful as a prognostic factor for BA patients with liver cirrhosis. In addition, fibrosis improved even after the development of cirrhosis.

31. Beta-D-Glucan Levels With Use of an Anti-adhesion Barrier Film in Pediatric Living Donor Liver Transplantation

Author

Ueno, Takehisa, Kodama, Tasuku, Noguchi, Yuki, Deguchi, Koichi, Nomura, Motonari, Saka, Ryuta, Watanabe, Miho, Tazuke, Yuko, Bessho, Kazuhiko, Okuyama, Hiroomi, Ueno, Takehisa, Kodama, Tasuku, Noguchi, Yuki, Deguchi, Koichi, Nomura, Motonari, Saka, Ryuta, Watanabe, Miho, Tazuke, Yuko, Bessho, Kazuhiko, and Okuyama, Hiroomi

Abstract

Ueno T., Kodama T., Noguchi Y., et al. Beta-D-Glucan Levels With Use of an Anti-adhesion Barrier Film in Pediatric Living Donor Liver Transplantation. Transplantation Proceedings 52, 1818 (2020); https://doi.org/10.1016/j.transproceed.2020.02.147., Introduction: Serum beta-D-glucan (BDG) levels may increase with anti-adhesion barrier film (ABF) use during pediatric living donor liver transplantation (LDLT). It may affect detection of fungal infections after LDLT. We evaluate BDG levels after pediatric LDLT. Methods: Pediatric patients who received an ABF during LDLT were included. Patients who may have had fungal infections prior to LDLT were excluded. One sheet of ABF was placed in the peritoneum during abdominal closure. Serum BDG levels before transplantation and on postoperative days (PODs) 1, 4, 7, 14, 21, and 28 and peritoneal fluid BDG levels on PODs 1 and 7 were measured. Results: Sixteen patients received an ABF during LDLT. Median age at transplant was 1.9 years (range, 6-11 years). Median body weight was 12.6 kg (range, 6.8-39 kg). Indications for LDLT were biliary atresia (n = 10) and other (n = 5). Prior to transplantation, the mean serum BDG level was 3.8 pg/mL. Mean Serum BDG levels were 18.1, 38.3, 5.3, 3.8, 3.3, and 3.3 pg/mL on PODs 1, 4, 7, 14, 21, and 28, respectively. Mean peritoneal fluid BDG levels were 485.9 and 240.4 pg/mL on PODs 1 and 7, respectively. No clinical fungal infections were observed. Conclusions: BDG levels were high in serum and peritoneal fluid after pediatric LDLT. Serum BDG levels normalized after POD 7. Careful interpretation of BDG levels until POD 7 is needed when an ABF has been used.

32. Impact of Monosegment Graft Use for Infants in Pediatric Living Donor Liver Transplantation

Author

Ueno, Takehisa, Toyama, Chiyoshi, Deguchi, Koichi, Masahata, Kazunori, Nomura, Motonari, Watanabe, Miho, Kamiyama, Masafumi, Tazuke, Yuko, Bessho, Kazuhiko, Okuyama, Hiroomi, Ueno, Takehisa, Toyama, Chiyoshi, Deguchi, Koichi, Masahata, Kazunori, Nomura, Motonari, Watanabe, Miho, Kamiyama, Masafumi, Tazuke, Yuko, Bessho, Kazuhiko, and Okuyama, Hiroomi

Abstract

Ueno T., Toyama C., Deguchi K., et al. Impact of Monosegment Graft Use for Infants in Pediatric Living Donor Liver Transplantation. Transplantation Proceedings 54, 391 (2022); https://doi.org/10.1016/j.transproceed.2021.12.034., Background: Left lateral segment grafts are generally used for very young pediatric patients undergoing living donor liver transplantation (LDLT). Recently, graft reduction techniques were developed for LDLT. Monosegment grafting has been used in newborns. The aim of this study was to determine the usefulness of monosegment grafting for infants. Methods: Recipients <2 years of age who underwent LDLT with a monosegment graft between 2010 and 2020 were gathered. Parents comprised all LDLT donors. A segment 2 monosegment graft was resected as a graft from the donor. Standard liver volume (SLV) was estimated using Urata's equation. Graft type, graft weight (GW), and native liver weight were assessed. Results: Eight patients were included in the study. Original diseases consisted of biliary atresia (n = 6) and fulminant hepatitis (n = 2). Final graft type included monosegment (n = 5) and reduced monosegment (n = 3). Median final GW/body weight after reduction was 3% (range, 2%-3.4%). Median native liver weight/SLV was 134% except in patients with fulminant hepatitis. Median pre-reduction graft volume (GV)/estimated GV was 113% (range, 60%-208%). Median pre-reduction GV/SLV of monosegment grafts that required reduction (n = 3) was 109% (range, 106%-121%). Median final reduced graft GV/SLV was 80% (range, 74%-91%). Complications due to large-for-size grafts were not observed. One case of bile leakage due to graft reduction occurred as a complication. Grafts were functioning well with the exception of one graft loss due to antibody-mediated rejection. Conclusion: Estimated GV in infants varies widely. Monosegment grafting can be useful for infants as well as newborns.

33. Long-Term Outcome of Portal Vein Stenting After Pediatric Living Donor Liver Transplantation

Author

Ueno, Takehisa, Toyama, Chiyoshi, Deguchi, Koichi, Masahata, Kazunori, Nomura, Motonari, Watanabe, Miho, Kamiyama, Masafumi, Tazuke, Yuko, Bessho, Kazuhiko, Okuyama, Hiroomi, Ueno, Takehisa, Toyama, Chiyoshi, Deguchi, Koichi, Masahata, Kazunori, Nomura, Motonari, Watanabe, Miho, Kamiyama, Masafumi, Tazuke, Yuko, Bessho, Kazuhiko, and Okuyama, Hiroomi

Abstract

Ueno T., Toyama C., Deguchi K., et al. Long-Term Outcome of Portal Vein Stenting After Pediatric Living Donor Liver Transplantation. Transplantation Proceedings 54, 454 (2022); https://doi.org/10.1016/j.transproceed.2022.01.008., Background: Portal vein (PV) stenosis is sometimes seen in pediatric living donor liver transplantation (LDLT). PV stents have been attempted in adults with persistent stenosis. However, long-term usefulness of PV stenting is unknown because stents do not expand with growth. We investigated the effect and long-term outcome of PV stenting for stenosis after pediatric LDLT. Methods: We included patients aged <18 years who underwent LDLT from 1998 to 2020 and who underwent PV stenting for stenosis. We assessed age at procedure, stent complications, and long-term outcomes. Results: Five patients underwent PV stent placement. The median age at LDLT was 10 years (range, 0.8-18.1 years). The median interval between LDLT and stent placement was 25 months. The median age at stent placement was 16 years (range, 3-20 years). The median body weight was 38 kg (range, 13-63 kg). The median stent diameter was 8 mm. The median observation period after stent placement was 8 years. On average, body weight increased 1.6 times. One complication associated with stent placement was PV thrombosis, which resulted in stent failure, but we observed no portal hypertension. In the other 4 patients, the stent has remained functioning, and there was no clinical evidence of portal hypertension. Conclusions: PV stents are effective for intractable PV stenosis in children. PV stents were successfully placed in children as young as 3 years old and weighing 13 kg. Our data suggests that a stent placed in young children does not cause portal hypertension as patients grow.

34. Early Use of Everolimus as a Third Immunosuppressive Agent for Intestinal Transplantation: A Report of 2 Cases

Author

Ueno, Takehisa, Toyama, Chiyoshi, Deguchi, Koichi, Masahata, Kazunori, Nomura, Motonari, Watanabe, Miho, Kamiyama, Masafumi, Tazuke, Yuko, Bessho, Kazuhiko, Okuyama, Hiroomi, Ueno, Takehisa, Toyama, Chiyoshi, Deguchi, Koichi, Masahata, Kazunori, Nomura, Motonari, Watanabe, Miho, Kamiyama, Masafumi, Tazuke, Yuko, Bessho, Kazuhiko, and Okuyama, Hiroomi

Abstract

Ueno T., Toyama C., Deguchi K., et al. Early Use of Everolimus as a Third Immunosuppressive Agent for Intestinal Transplantation: A Report of 2 Cases. Transplantation Proceedings 54, 472 (2022); https://doi.org/10.1016/j.transproceed.2022.01.010., Background: In patients with intestinal transplantation (ITx), renal function is easily impaired because of long-term parenteral nutrition and side effects of tacrolimus. Everolimus was used in patients with renal insufficiency in our study. Methods: We administered everolimus as a third immunosuppressive agent in addition to tacrolimus and steroids for renal sparing in patients who received ITx. We assessed everolimus levels, complications, and renal function. Results: Two patients received everolimus after ITx. Patient 1 was a 13-year-old boy who underwent ITx for an allied disorder of Hirschsprung's disease. After induction therapy with rabbit antithymocyte globulin, maintenance therapy consisted of tacrolimus and steroids. Everolimus was introduced 3 months after ITx for renal sparing. Seven months later, the patient required partial intestinal graft resection owing to bowel obstruction. Everolimus was suspended for only 2 weeks. Four years after ITx, the trough level of tacrolimus was maintained at 3 to 5 ng/mL. The trough level of everolimus was maintained at 3 to 5 ng/mL. Patient 2 was a 32-year-old man who underwent deceased ITx for short gut syndrome. Induction and maintenance immunosuppression was the same as for patient 1. Everolimus was introduced 1 month after surgery. Two years after ITx, trough levels of tacrolimus and everolimus were the same as in patient 1. No rejection was observed in either patient, and renal function was well maintained. We observed no side effects caused by everolimus. Conclusions: Everolimus could be used safely and effectively after ITx. Early use of everolimus after ITx did not affect wound healing.

35. Clinical implications of serum autotoxin in regular follow up after pediatric living donor liver transplantation for biliary atresia

Author

Ueno, Takehisa, Takase, Koki, Toyama, Chiyoshi, Deguchi, Koichi, Masahata, Kazunori, Nomura, Motonari, Watanabe, Miho, Kamiyama, Masafumi, Tazuke, Yuko, Bessho, Kazuhiko, Okuyama, Hiroomi, Ueno, Takehisa, Takase, Koki, Toyama, Chiyoshi, Deguchi, Koichi, Masahata, Kazunori, Nomura, Motonari, Watanabe, Miho, Kamiyama, Masafumi, Tazuke, Yuko, Bessho, Kazuhiko, and Okuyama, Hiroomi

Abstract

Background: : Pediatric patients sometimes develop graft fibrosis after living donor liver transplant (LDLT). Autotaxin is a recently developed serum marker for hepatic fibrosis. We studied the relationship between serum autotaxin levels and histological findings in patients after LDLT for biliary atresia (BA). Methods: Information on patients aged <19 years who received LDLT for BA and were followed for at least 1 year after LDLT was gathered. Autotaxin levels were compared with pathological fibrosis scores. Results: The study included 52 patients, of whom 4 patients had no fibrosis (F0), 36 patients had F1 fibrosis, and 12 patients had F2. The median serum autotaxin level was 0.89 mg/L. In patients with portal vein (PV) complications such as stenosis or thrombosis (n = 7), the mean autotoxin level was 1.25 mg/L compared with 0.95 mg/L in patients without PV complications (p = 0.004). Among patients without PV complications, the mean autotaxin level was 0.90, 0.88, and 1.18 mg/L in F0, F1, and F2 fibrosis, respectively. The mean autotaxin was higher in F2 fibrosis than in F0 or F1 fibrosis (p<0.05). Autotoxin had a high area under the curve (0.86) with the cut-off level of 0.897 mg/L. Conclusion: Serum autotaxin is a novel marker for liver fibrosis in patients after pediatric LDLT for BA. Type of study: : Study of Diagnostic Test. Level of evidence: : Level II.

36. Clinical implications of serum autotoxin in regular follow up after pediatric living donor liver transplantation for biliary atresia

Author

Ueno, Takehisa, Takase, Koki, Toyama, Chiyoshi, Deguchi, Koichi, Masahata, Kazunori, Nomura, Motonari, Watanabe, Miho, Kamiyama, Masafumi, Tazuke, Yuko, Bessho, Kazuhiko, Okuyama, Hiroomi, Ueno, Takehisa, Takase, Koki, Toyama, Chiyoshi, Deguchi, Koichi, Masahata, Kazunori, Nomura, Motonari, Watanabe, Miho, Kamiyama, Masafumi, Tazuke, Yuko, Bessho, Kazuhiko, and Okuyama, Hiroomi

Abstract

Background: : Pediatric patients sometimes develop graft fibrosis after living donor liver transplant (LDLT). Autotaxin is a recently developed serum marker for hepatic fibrosis. We studied the relationship between serum autotaxin levels and histological findings in patients after LDLT for biliary atresia (BA). Methods: Information on patients aged <19 years who received LDLT for BA and were followed for at least 1 year after LDLT was gathered. Autotaxin levels were compared with pathological fibrosis scores. Results: The study included 52 patients, of whom 4 patients had no fibrosis (F0), 36 patients had F1 fibrosis, and 12 patients had F2. The median serum autotaxin level was 0.89 mg/L. In patients with portal vein (PV) complications such as stenosis or thrombosis (n = 7), the mean autotoxin level was 1.25 mg/L compared with 0.95 mg/L in patients without PV complications (p = 0.004). Among patients without PV complications, the mean autotaxin level was 0.90, 0.88, and 1.18 mg/L in F0, F1, and F2 fibrosis, respectively. The mean autotaxin was higher in F2 fibrosis than in F0 or F1 fibrosis (p<0.05). Autotoxin had a high area under the curve (0.86) with the cut-off level of 0.897 mg/L. Conclusion: Serum autotaxin is a novel marker for liver fibrosis in patients after pediatric LDLT for BA. Type of study: : Study of Diagnostic Test. Level of evidence: : Level II.

37. Treatment and follow-up of late onset intra hepatic bile duct stones in congenital biliary dilatation

Author

Ueno, Takehisa, Deguchi, Koichi, Masahata, Kazunori, Nomura, Motonari, Watanabe, Miho, Kamiyama, Masafumi, Tazuke, Yuko, Yoshioka, Teppei, Nose, Satoko, Okuyama, Hiroomi, Ueno, Takehisa, Deguchi, Koichi, Masahata, Kazunori, Nomura, Motonari, Watanabe, Miho, Kamiyama, Masafumi, Tazuke, Yuko, Yoshioka, Teppei, Nose, Satoko, and Okuyama, Hiroomi

Abstract

This version of the article has been accepted for publication, after peer review (when applicable) and is subject to Springer Nature’s AM terms of use, but is not the Version of Record and does not reflect post-acceptance improvements, or any corrections. The Version of Record is available online at: https://doi.org/10.1007/s00383-022-05321-w., Purpose: The postoperative course after surgery for congenital biliary dilatation (CBD) has some complications. Intrahepatic bile duct (IHBD) stones were known as a late complication. We report on the treatment and long-term follow-up of postoperative IHBD stones in our department. Methods: Patients who underwent CBD surgery at age 15 years or younger in our department were identified. Those followed up for 5 years or more were enrolled. Annual blood chemistry tests and abdominal ultrasonography were performed. Each patient’s surgical procedure, IHBD stone diagnosis, treatments, and outcomes were retrospectively assessed. Results: Fifty-one patients were analyzed. The median age at the last visit was 24 years (range 7–45 years), and the median age at CBD surgery was 3 years. Eight patients (16%) developed late-onset IHBD stones. The median age at onset was 25 years, and the median duration after surgery was 20 years. The initial treatment was double-balloon enteroscopy (DBE) in 4 cases, which resulted in stone removal in 3 of the 4 patients (75%). Conclusion: Since CBD may cause late-onset IHBD stones, continuous follow-up is required even in adulthood. In this study, DBE was effective and minimally invasive, and it is recommended as the initial treatment.

38. Plasma Concentration of Antifungal Agent Micafungin for Pediatric Living Donor Liver Transplantation

Author

Ueno, Takehisa, Takase, Koki, Deguchi, Koichi, Nomura, Motonari, Watanabe, Miho, Kamiyama, Masafumi, Tazuke, Yuko, Kimura, Takeshi, Okuyama, Hiroomi, Ueno, Takehisa, Takase, Koki, Deguchi, Koichi, Nomura, Motonari, Watanabe, Miho, Kamiyama, Masafumi, Tazuke, Yuko, Kimura, Takeshi, and Okuyama, Hiroomi

Abstract

Ueno T., Takase K., Deguchi K., et al. Plasma Concentration of Antifungal Agent Micafungin for Pediatric Living Donor Liver Transplantation. Transplantation Proceedings 56, 602 (2024); https://doi.org/10.1016/j.transproceed.2024.01.020., Background: Pediatric living-donor liver transplantation (LDLT) candidates often receive long-term antibiotic treatment. Micafungin has been used as an antifungal agent after LDLT, but the adequate dose after pediatric LDLT was unknown. Here, we report micafungin blood concentrations after pediatric LDLT and discuss its safety and adequate dosing. Methods: Pediatric patients with data on micafungin concentrations after LDLT were identified. Those with surgical complications were excluded. All patients received standard tacrolimus-based immunosuppression. A micafungin dose of 1 mg/kg was administered once daily for 10 days starting on postoperative day (POD) 1. The trough and peak micafungin blood concentrations were evaluated on PODs 1, 4, 7, and 10. Beta D glucan levels and liver function tests were assessed to determine micafungin effectiveness and safety. Results: Ten patients were enrolled, with a median age of 1.2 years. The median graft vs body weight ratio was 2.7%. The primary diseases were biliary atresia (n = 7), Alagille syndrome (n = 2), and progressive familial intrahepatic cholestasis type 2 (n = 1). Mean peak micafungin levels were 4.47, 6.27, 5.47, and 5.47 µg/mL on PODs 1, 4, 7, and 10, respectively. Mean trough levels were 2.03, 1.88, and 2.66 µg/mL on PODs 4, 7, and 10, respectively. The micafungin half-lives were 13.7, 14.7, and 14.0 hours on PODs 4, 7, and 10, respectively. Beta D glucan levels were 4.4 pg/mL and 3.7 pg/mL before and after transplantation, respectively, indicating no significant difference (P = .3). No clinical fungal infections were observed. Conclusion: Micafungin administration is safe and effective after pediatric LDLT.

39. Impact of Total Parenteral Nutrition on Preoperative Management of Pediatric Living-Donor Liver Transplantation for Biliary Atresia Under 2 Years Old

Author

Ueno, Takehisa, Takase, Koki, Deguchi, Koichi, Nomura, Motonari, Watanabe, Miho, Kamiyama, Masafumi, Tazuke, Yuko, Kimura, Takeshi, Okuyama, Hiroomi, Ueno, Takehisa, Takase, Koki, Deguchi, Koichi, Nomura, Motonari, Watanabe, Miho, Kamiyama, Masafumi, Tazuke, Yuko, Kimura, Takeshi, and Okuyama, Hiroomi

Abstract

Ueno T., Takase K., Deguchi K., et al. Impact of Total Parenteral Nutrition on Preoperative Management of Pediatric Living-Donor Liver Transplantation for Biliary Atresia Under 2 Years Old. Transplantation Proceedings 56, 605 (2024); https://doi.org/10.1016/j.transproceed.2024.01.017., Background: Liver failure and gastrointestinal bleeding occur in the end-stage of biliary atresia (BA). Living-donor liver transplantation (LDLT) is a standard treatment in Japan. Our program actively provides pre-transplant total parenteral nutrition (TPN) for such patients, and here we report its efficiency and safety. Methods: Patients with BA for whom LDLT was indicated were identified. Those with a long-term external central venous catheter and TPN, longer than 4 weeks before LDLT, were analyzed. Ascites was controlled with diuretics. TPN indications, efficacy, and complications were assessed along with patient growth, biochemical markers, and gastrointestinal bleeding. Results: Fourteen patients were included in the study, of whom 8 were girls and 6 were boys. The median age at LDLT was 0.9 years. Body weight (BW) at TPN initiation averaged 6799 g, and the median serum total bilirubin was 9.5 mg per dL. The median catheterization duration was 54 days, and 1 patient received home TPN. Indications for TPN were gastrointestinal bleeding and/or massive esophageal varices in 4 patients and poor nutritional status in 10 patients. No complications were observed except for 1 catheter infection and 1 catheter occlusion. The median final body weight before LDLT was 7906 g. The mean rate of BW gain was significantly higher after TPN than before (149 vs 32 g/wk, respectively, P = .0002). Mean prothrombin time and levels of albumin, cholinesterase, and total bilirubin were not significantly different at the start and end of TPN. Conclusions: Pre-transplant TPN was safe and effective for patients with end-stage BA.

40. Effect of microscopy-assisted portoenterostomy (MAPE) for biliary atresia

Author

Ueno, Takehisa, Kodama, Tasuku, Noguchi, Yuki, Nomura, Motonari, Saka, Ryuta, Takama, Yuichi, Tazuke, Yuko, Bessho, Kazuhiko, Okuyama, Hiroomi, Ueno, Takehisa, Kodama, Tasuku, Noguchi, Yuki, Nomura, Motonari, Saka, Ryuta, Takama, Yuichi, Tazuke, Yuko, Bessho, Kazuhiko, and Okuyama, Hiroomi

Abstract

This version of the article has been accepted for publication, after peer review (when applicable) and is subject to Springer Nature’s AM terms of use, but is not the Version of Record and does not reflect post-acceptance improvements, or any corrections. The Version of Record is available online at: https://doi.org/10.1007/s00383-020-04794-x., Purpose: Portoenterostomy (PE) is the standard treatment for biliary atresia (BA). However, micro-bile ducts are difficult to identify with surgical loupes and dissect systematically. We report the effects of our attempts to dissect hilar tissue using a surgical microscope. Methods: Microscopy-assisted portoenterostomy (MAPE) was initiated in 2014. Patients born between 2000 and 2013 who underwent PE until day 70 without a surgical microscope for BA were gathered as historical control. MAPE in re-do PE cases (Re-MAPE) was evaluated in the same manner. Results: Ten patients underwent MAPE for BA during the study period. 17 patients in the conventional PE group were gathered. In the MAPE group, the jaundice clearance rate was 80%, compared with 53% in the conventional PE group. Re-MAPE was performed in four patients, who had a jaundice clearance rate of 75%, essentially identical to the rate with initial MAPE. At age 4 years, the native liver survival rate was 58% in the MAPE group and 38% in the conventional PE group. The native liver survival rate in the Re-MAPE group was 75%. Conclusion: MAPE is useful for sharing the surgical field during open PE in patients with BA. It may improve the rate of jaundice clearance.

41. Balloon dilatation for congenital esophageal stenosis associated with esophageal atresia

Author

Deguchi, Koichi, Kamiyama, Masafumi, Masahata, Kazunori, Nomura, Motonari, Watanabe, Miho, Ueno, Takehisa, Tazuke, Yuko, Okuyama, Hiroomi, Deguchi, Koichi, Kamiyama, Masafumi, Masahata, Kazunori, Nomura, Motonari, Watanabe, Miho, Ueno, Takehisa, Tazuke, Yuko, and Okuyama, Hiroomi

Abstract

The version of record of this article, first published in Pediatric Surgery International, is available online at Publisher’s website: https://doi.org/10.1007/s00383-024-05652-w., Purpose: Congenital esophageal stenosis (CES) associated with esophageal atresia (EA) is rare, and no standard treatment has been established. We reviewed cases of EA-associated CES to assess the clinical characteristics and treatment outcomes, especially the feasibility of endoscopic dilatation. Methods: We retrospectively examined patients with EA-associated CES. We also compared treatment outcomes of EA-associated CES with those of EA patients without CES who developed postoperative anastomotic stricture. Results: Among 44 patients with EA, ten had CES (23%). Postoperative complications were not significantly different between EA patients with CES and those without CES but with anastomotic stricture. All CES patients underwent balloon dilatation as initial treatment. Eight of nine patients (89%) were successfully treated by dilatation only, and one patient underwent surgical resection. The median number of balloon dilatations for CES was five (2–17), which was higher than that for anastomotic stricture in patients without CES (p = 0.012). Esophageal perforation occurred in five patients with CES (5/9, 56%) after dilatation, but all perforations were successfully managed conservatively with an uneventful post-dilatation course. Conclusions: Twenty-three percent of patients with EA had CES. Although balloon dilatation for EA-associated CES required multiple treatments and carried a risk of perforation, balloon dilatation showed an 89% success rate and all perforations could be managed conservatively.

42. Tegavivint and the β-Catenin/ALDH Axis in Chemotherapy-Resistant and Metastatic Osteosarcoma.

Author

Nomura M, Rainusso N, Lee YC, Dawson B, Coarfa C, Han R, Larson JL, Shuck R, Kurenbekova L, and Yustein JT

Subjects
Animals, Apoptosis, Biomarkers, Tumor metabolism, Bone Neoplasms drug therapy, Bone Neoplasms metabolism, Bone Neoplasms pathology, Cell Proliferation, Enzyme Inhibitors pharmacology, Female, Humans, Lung Neoplasms metabolism, Lung Neoplasms secondary, Male, Mice, Mice, Inbred NOD, Mice, SCID, Osteosarcoma metabolism, Osteosarcoma pathology, Tumor Cells, Cultured, Xenograft Model Antitumor Assays, beta Catenin metabolism, Aldehyde Dehydrogenase antagonists & inhibitors, Antineoplastic Agents pharmacology, Drug Resistance, Neoplasm drug effects, Gene Expression Regulation, Neoplastic drug effects, Lung Neoplasms drug therapy, Osteosarcoma drug therapy, beta Catenin antagonists & inhibitors
Abstract

Background: The Wnt/β-catenin pathway is closely associated with osteosarcoma (OS) development and metastatic progression. We investigated the antitumor activity of Tegavivint, a novel β-catenin/transducin β-like protein 1 (TBL1) inhibitor, against OS employing in vitro, ex vivo, and in vivo cell line and patient-derived xenograft (PDX) models that recapitulate high risk disease., Methods: The antitumor efficacy of Tegavivint was evaluated in vitro using established OS and PDX-derived cell lines. Use of an ex vivo three-dimensional pulmonary metastasis assay assessed targeting of β-catenin activity during micro- and macrometastatic development. The in vivo activity of Tegavivint was evaluated using chemoresistant and metastatic OS PDX models. Gene and protein expression were quantified by quantitative Reverse transcription polymerase chain reaction or immunoblot analysis. Bone integrity was determined via microCT. All statistical tests were two-sided., Results: Tegavivint exhibited antiproliferative activity against OS cells in vitro and actively reduced micro- and macrometastatic development ex vivo. Multiple OS PDX tumors (n = 3), including paired patient primary and lung metastatic tumors with inherent chemoresistance, were suppressed by Tegavivint in vivo. We identified that metastatic lung OS cell lines (n = 2) exhibited increased stem cell signatures, including enhanced concomitant aldehyde dehydrogenase (ALDH1) and β-catenin expression and downstream activity, which were suppressed by Tegavivint (ALDH1: control group, mean relative mRNA expression = 1.00, 95% confidence interval [CI] = 0.68 to 1.22 vs Tegavivint group, mean = 0.011, 95% CI = 0.0012 to 0.056, P < .001; β-catenin: control group, mean relative mRNA expression = 1.00, 95% CI = 0.71 to 1.36 vs Tegavivint group, mean = 0.45, 95% CI = 0.36 to 0.52, P < .001). ALDH1high PDX-derived lung OS cells, which demonstrated enhanced metastatic potential compared with ALDHlow cells in vivo, were sensitive to Tegavivint. Toxicity studies revealed decreased bone density in male Tegavivint-treated mice (n = 4 mice per group)., Conclusions: Tegavivint is a promising therapeutic agent for advanced stages of OS via its targeting of the β-catenin/ALDH1 axis., (© The Author(s) 2019. Published by Oxford University Press. All rights reserved. For permissions, please email: journals.permissions@oup.com.)

Published
2019
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