17 research outputs found
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Simultaneous Liver and Pancreas Transplantation in Patients With Cystic Fibrosis
Improved survival in patients with cystic fibrosis (CF) has led to an increased incidence of extrapulmonary complications of this disease. Of these, cirrhosis and pancreatic insufficiency, including CF-related diabetes (CFRD) and exocrine insufficiency, are significant causes of morbidity and mortality. Liver transplantation is the treatment of choice for cirrhosis in this setting, but the addition of an isolated simultaneous pancreas transplant in patients with CFRD has not been reported.
Two female patients with CF underwent simultaneous pancreas and liver transplantation. Both had pancreatic insufficiency, CFRD, cirrhosis, and preserved renal function. In each case, the liver and pancreas were procured from a single cadaveric donor. The liver transplant was performed first. A lower midline extension was added for improved exposure of the iliac vessels. The donor pancreas transplant was performed with systemic venous drainage and enteric exocrine drainage. Immunosuppression included rabbit anti-thymocyte globulin, tacrolimus, mycophenolate mofetil, and early steroid withdrawal.
Both patients recovered well with normal liver function, resolution of portal hypertension, and normal blood glucoses independent of insulin. As a result of the enteric exocrine drainage of the pancreas, they are now independent of supplemental pancreatic enzymes.
Simultaneous liver and pancreas transplantation in CF patients provides the advantages of normalization of glucose and improved nutrition for patients requiring liver transplantation and should be considered in CF patients with CFRD who require liver transplants
Liver transplantation after radioembolization in a patient with unresectable HCC
Background. A 58-year-old white man who was being followed by his hepatologist for nonalcoholic steatohepatitis-related liver cirrhosis and portal hypertension and who had been found to have a biopsy-proven hepatocellular carcinoma (HCC) on routine screening, self-referred to our center for a second opinion on the management of his HCC. Investigations. Laboratory investigations, CT scan of the abdomen and chest, bone scan and technetium macroaggregated albumin scan. Diagnosis. The patient had unresectable HCC. Management. The patient underwent two treatments with Yttrium-90 glass microspheres, which were performed as outpatient procedures 1 month and 3 months after diagnosis. He underwent orthotopic liver transplantation (OLT) 1 year after the initial diagnosis of HCC. The post-OLT immunoregimen included OKT3 plus rituximab and high-dose steroids. On discharge from hospital he was on immunosuppressive treatment with tacrolimus. He had de novo autoimmune hepatitis 6 months post-OLT, which was treated with a short course of low-dose steroids and addition of mycophenolate mofetil
New direct-acting antivirals in the development for hepatitis C virus infection
A large number of new therapies are in development for chronic hepatitis C
including direct-acting antiviral drugs (DAA), which target specific hepatitis C
virus enzymes. Two of these compounds have already advanced into phase 3
development in the USA and EU, and many more are in phase 2 trials and likely to
advance. In this review, the results of recent studies on ribavirin analogues,
nonstructural (NS) 3/4 serine protease inhibitors, NS5B polymerase inhibitors,
cyclophilin inhibitors, silimarin components, and thiazolides have been updated.
Each compound includes a brief summary of its proposed mechanism of action,
results of early clinical trials, and more advanced trial data where available.
These compounds are likely to be the first approved in the USA and EU and will
initially be used in combination with the current standard of care. It is
possible that future treatment paradigms with these agents will offer the
potential of interferon-free regimens. It is most likely that patients for these
new therapies will be selected carefully by identifying and treating first those
who have excellent sustained virologic response rates with 24 weeks of pegylated
interferon and ribavirin, the current standard of care. It is also likely that
there will be a need to identify those patients who are not likely to have a
sustained virologic response with the addition of a protease inhibitor to the
current standard of care and delaying their therapy until combination viral
suppression therapy becomes an option. The cost and side effects of the DAA will
be important considerations for treating physicians. This review is current
through 2009; however, data are rapidly changing
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[649] CPG 10101 (ACTILON) IN COMBINATION WITH PEGYLATED INTERFERON AND/OR RIBAVIRIN IN CHRONIC HCV GENOTYPE 1 INFECTED PATIENTS WITH PRIOR RELAPSED RESPONSE: WEEK 48 DATA
Elbasvir/Grazoprevir
Each month, subscribers to The Formulary Monograph Service receive 5 to 6 well-documented monographs on drugs that are newly released or are in late phase 3 trials. The monographs are targeted to Pharmacy & Therapeutics Committees. Subscribers also receive monthly 1-page summary monographs on agents that are useful for agendas and pharmacy/nursing in-services. A comprehensive target drug utilization evaluation/medication use evaluation (DUE/MUE) is also provided each month. With a subscription, the monographs are available online to subscribers. Monographs can be customized to meet the needs of a facility. Through the cooperation of The Formulary, Hospital Pharmacy publishes selected reviews in this column. For more information about The Formulary Monograph Service, contact Wolters Kluwer customer service at 866-397-3433. The September 2016 monograph topics are barictinib, buprenorphine implants, sarilumab, sofosbuvir/velpatasvir, and cholera vaccine, live, oral. The Safey MUE is on sofosbuvir/velpatasvir