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How renal impairment impacts postoperative spine surgery morbidity — 6 key ... - Becker's Orthopedic Spine |
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The study is a large, multicenter, clinical registry that gathered data on lumbar spine surgery patients in 2012. There were 13,576 cases included in the study. The researchers found:
1. The morbidity risk increased with a worsening estimated glomerular filtration rate in the inverse-logarithmic fashion. The risk magnitude increased substantially for patients with eGRF below 60.
2. There was a 26 percent relative increase in morbidity in moderate to severe renal impairment patients. This is compared with the propensity score—matched cohort of patients with no or mild disease.
3. The wound complication rates were higher in patients with moderate or severe disease, 3 percent versus 2.1 percent.
4. Reoperation rates were higher — 4.6 percent — in the patients with moderate or severe disease than the patients without — 3.3 percent.
5. Blood transfusions were higher — 16.3 percent — among patients with moderate or severe disease, as compared with patients who didn’t have disease — 12.8 percent.
6. The patients with a preoperative moderate or severe renal impairment were 10 times more likely to develop acute renal failure after surgery, according to the report.
The researchers concluded the 30-day morbidity risk after lumbar spine surgery was strongly associated with renal impairment. “These data may be useful for preoperative patient counseling and patients with severe renal disease, particularly in elective cases,” concluded the study authors.
More articles on spine surgery:
Spinal cord injuries rising among the elderly—5 facts to note
Tidelands Health names Dr. T. Scott Ellison to board of trustees
Spine surgery’s RTCs are fragile
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Hepatitis C and End Stage Renal Disease - Healio |
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Hepatitis C is a major cause of morbidity and mortality in patients with end stage renal disease and kidney transplant candidates. The prevalence of positive HCV antibody in patients on hemodialysis ranges from 5% to 60% in developed countries, depending on other risk factors. The spread of HCV in dialysis centers is declining, but hemodialysis remains a risk factor for viral hepatitis and is included in the CDC screening guidelines as a risk factor that warrants HCV screening.
Catherine T. Frenette
It has been well-shown that HCV positive patients with ESRD have increased liver-related mortality and all-cause mortality. Patients with HCV who are on the kidney transplant wait list also have increased risk of death, especially with coexisting diabetes. After kidney transplantation, the risk of death from liver disease in someone with hepatitis C is 21%, compared to 0% if patients are not infected with hepatitis C.
Treatment has historically been difficult in this patient population. Treatment prior to kidney transplant or while on hemodialysis reduces the likelihood of HCV-related complications and death. However, use of interferon in patients who are chronically ill is fraught with complications. In addition, ribavirin is predominantly cleared renally, and in patients with ESRD the use of ribavirin can be associated with significant anemia. Treatment after kidney transplant in the interferon era was associated with a high risk of graft rejection and potential graft loss. Sustained virologic response rates for interferon-based therapies in this patient population have been reported ranging from 13% to 75%.
The use of new direct-acting antivirals in the setting of severe renal disease, ESRD and hemodialysis is currently under investigation. As of now, most of the studies have been with patients on hemodialysis rather than peritoneal dialysis. Several abstracts have been presented at national and international meetings that address the need of dosing guidance for DAAs in the setting of renal disease.
DAA Metabolism and Use in Renal Failure
Simeprevir
The elimination of simeprevir (Olysio, Janssen) occurs via biliary excretion, and renal clearance plays an insignificant role in its elimination. No dose adjustment is required for mild, moderate or severe renal impairment. Per the package insert, the safety and efficacy has not been established in patients with creatinine clearance (CrCl) below 30 mL/min or in patients on hemodialysis.
Sofosbuvir
Sofosbuvir (Sovaldi, Gilead Sciences) is metabolized in the liver to form the pharmacologically active nucleoside analog triphosphate GS-461203. Dephosphorylation of this moiety results in the formation of the nucleoside metabolite GS-331007, which has no antiviral activity. This metabolite GS-331007 is cleared in the urine, and thus dose adjustments may be required in patients with ESRD. The area under the curve (AUC) of sofosbuvir is 2.7-fold higher in patients with severe renal impairment (CrCl < 30), and the AUC of GS-331007 is 5.5-fold higher than in patients without renal impairment. Per the package insert, the safety and efficacy has not been established in patients with CrCl below 30 mL/min or in patients on hemodialysis.
Ledipasvir
No detectable metabolism of ledipasvir (Gilead Sciences) is observed by the cytochrome P450 enzymes. Evidence of slow oxidative metabolism via an unknown mechanism has been observed. Ledipasvir is predominantly excreted in the feces, with renal excretion being a minor pathway. In patients with severe renal impairment, no pharmacokinetic differences were observed.
Ombitasvir, Paritaprevir/Ritonavir, and Dasabuvir
Ombitasvir is predominantly metabolized by amide hydrolysis followed by oxidative metabolism, and paritaprevir/ritonavir, and dasabuvir are metabolized by the cytochrome P450 system (Viekira Pak, AbbVie). All of these medications are predominantly excreted into the feces, with minimal renal excretion. In the package insert, dosing is unchanged for patients with CrCl above 15 mL/min. In clinical trials, it appears that dosing is also unchanged for patients on hemodialysis.
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New Data Immediately Changes Practice in Renal Failure, Decompensated ... - Healio |
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With new data presented at the International Liver Congress, practicing physicians now have the power to make informed recommendations for patients who were not included in original pivotal trials of direct-acting antiviral regimens, such as those in renal failure and with decompensated cirrhosis.
Ira M. Jacobson
For myself and other clinicians, the data that came out of EASL are transformative in terms of what we can now bring to the table with our patients with renal failure. Before the meeting, we really didn’t know what to do. We had no database on which to predicate our results and now we do.
As Michael R. Charlton, MD, FRCP, explains in his Take Home from the ILC, the RUBY-1 study showed that the combination of ombitasvir, paritaprevir and ritonavir plus dasabuvir (Viekira Pak, AbbVie) had a positive response among their 14 patients with renal failure, with further data to follow. Now we have a regimen that seems to bear out the prediction, based on previous pharmacokinetic studies, that these drugs should not cause any particular problems for renal failure patients. There were no new or unique side effects that hadn’t been seen before, though dose interruptions related to hemoglobin declines from the ribavirin were fairly frequent. Even more impressive results, based on a much larger number of patients, were seen in C-SURFER (cited in the Patient Profile from Catherine T. Frenette, MD, for the not-yet-approved regimen of grazoprevir/elbasvir (Merck).
This shows us that the agents can be used in a fairly routine way to treat these patients with this previously extraordinarily unmet need. The question of the hour is whether these drugs are ready to be put into patients without label amendments for any of the existing regimens. For now, it’s up to individual clinicians and their patients to determine if these data are sufficient to proceed.
For me, the question was answered when I saw a patient with genotype 4 the day I returned from Vienna. The patient has bridging fibrosis and he’s desperate to receive antiviral therapy because his nephrologist won’t give him a new kidney without being cured.
We know that from earlier studies that the 3D regimen is very effective in genotype 4 (even the regimen of ombitasvir/paritaprevir/ritonavir works well, especially with ribavirin), so I felt comfortable making a recommendation for this patient, who keenly desired treatment without further delay, that from my perspective there was enough data from the RUBY-1 study to give this regimen.
Given that there are variable levels of urgency in treating patients with renal failure, including the question of whether, as in my patient, their progression toward getting a kidney transplant is being delayed by ongoing viremia in the setting of advanced fibrosis, there’s room for individualization.
Thus, depending on one’s perspective, EASL was a turning point in conferring on us the ability to make decisions to treat some of these renal failure patients proactively without waiting for additional data. There have also been encouraging small case reports of patients receiving sofosbuvir in the setting of renal failure, but sofosbuvir is renally excreted and no dose has yet been established for, nor can a dosing recommendation be made in, patients with renal failure at the present time. The issue is being studied.
Additionally, the presentation of SOLAR-2 data reaffirmed the groundshaking paradigm shift initiated by the SOLAR-1 results in decompensated cirrhotics presented at AASLD 2014.
One came home from that earlier meeting with a radically different perspective to the management of patients with decompensated cirrhosis than one likely had going into the meeting. In Vienna, we saw nearly duplicate results in the SOLAR-2 study, affirming rates of SVR of 85% to 90% with ledipasvir/sofosbuvir combined with ribavirin, with 12 weeks of treatment appearing (much to my surprise) as effective as 24 weeks. Even if the cure rates are not quite at the 95% or higher levels to which we have become accustomed in less advanced liver disease, it is near miraculous that we can cure our sickest patients at a rate close to 90% with 12 weeks of therapy. For now, we don’t know whether we can avoid ribavirin in this population because all the treatment arms in both studies contained it.
But this data poses a new dilemma, brought up by Mitchell L. Shiffman, MD, in his Take Home, which is whether our capacity to cure decompensated cirrhotics necessarily means you should treat all them.
That may seem like a foolish question, but it’s really a profound dilemma, particularly with regards to the decompensated cirrhotics who are very advanced, such as Child Pugh C patients with very high MELD scores, eg, above 20 (most of the patients in the SOLAR studies had MELD scores less than 20). This is because patients may reach a “point of no return” at which it’s too late to salvage a patient’s quality of life or even their very life by curing them virologically and you may actually delay their ability to get a transplant by reducing the MELD score sufficiently to deprioritize the patient on the transplant list.
The potential to harm patients by delaying their ability to get a transplant even has the potential to come with medico-legal consequences. We are going to have to work very hard in the next couple of years in a rigorous systematic fashion to identify this point of no return beyond which, although counterintuitive, we should not institute this curative therapy even though we’re capable of curing the disease. Some patients may simply be better off if we defer antiviral therapy until after transplantation, especially since recent data have been extraordinarily encouraging with regard to outcomes of antiviral therapy in the post-transplant setting.
— Ira M. Jacobson, MD
Co-Chief Medical Editor
HCV Next
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Ernie Reyes Jr. Needs A Kidney Transplant; 'Ninja Turtles' Actor is 'Fighting ... - Headlines Global News |
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Ernie Reyes Jr. Needs A Kidney Transplant; ‘Ninja Turtles’ Actor is ‘Fighting For His Life’
Actor Ernie Reyes Jr. needs a kidney transplant, and his sister is asking for help to raise the money for the procedure.
By Staff Reporter | Jun 12, 2015 04:43 PM EDT
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 Ernie Reyes Jr. (Photo : Twitter Photo Section )
Actor Ernie Reyes Jr. needs a kidney transplant, and his sister Destiny Reyes took to GoFundMe to raise $75,000 for the procedure.
The 43-year-old "Teenage Mutant Ninja Turtles II: The Secret of the Ooze" star is said to be "fighting for his life" and was recently hospitalized in the ICU for kidney failure, according to Us Weekly.
 (Photo : Twitter Photo Section) Ernie Reyes Jr.
"Ernie is currently undergoing dialysis treatment 3 times per week for 4 hours a day while waiting for a kidney transplant," Destiny wrote on GoFundMe. "This is a very challenging time not only for Ernie Jr.'s immediate family, but a challenging time for our family as well."
"My brother has spent his entire childhood and adult life fighting in films and television, but now his battle has gone from the screen to reality, fighting for his life," she added.
"Regardless of where you have seen or heard of Ernie Reyes Jr., he has impacted peoples' lives all over the world through his extraordinary performances in television and film. Please be aware that he needs support during this time of need and recovery of his life."
Reyes starred in "Sidekicks" in the 1980s and the "Ninja Turtles" flick in 1991, and he also had roles in "Rush Hour 2" and "Indiana Jones and the Kingdom of the Crystal Skull."
"Much love to my sister @destikneee for starting a kidney transplant fund for me," Ernie tweeted. "I love you girl!"
He also posted on Instagram a mirror selfie showing himself shirtless and sporting a bandage, E! Online reported.
 (Photo : Twitter Photo Section) Ernie Reyes Jr.
"5:15am-On my way to dialysis. #nevergiveup #motivationmonday," the actor wrote.
Despite his ailment, Ernie is still working and is set to host an event at the 2015 Battle of Atlanta Martial Arts Tournament next weekend.
Friends and fans have been showing support through social media, and since the fundraiser began on June 5, 753 people have chipped in to raise more than $37,000.
"I don't know what I would do without all your love and support," he tweeted this week. "Thank you from the bottom of my heart. #grateful."
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