Phase I and Pharmacokinetic Study of Sorafenib in Patients With Hepatic or Renal Dysfunction: CALGB 60301

Miller, Antonius A.; Murry, Daryl J.; Owzar, Kouros; Hollis, Donna; Abou‐Alfa, Ghassan K.; Desai, Apurva A.; Hwang, Jimmy J.; Villalona‐Calero, Miguel A.; Dees, E. Claire; Lewis, Lionel D.; Fakih, Marwan; Edelman, Martin J.; Millard, Fred; Frank, Richard C.; Hohl, Raymond J.; Ratain, Mark J.

doi:10.1200/jco.2008.20.0931

Cited by 195 publications

(155 citation statements)

References 24 publications

(19 reference statements)

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“…In this context, it is insightful to consider a pharmacokinetic study of sorafenib by Miller and colleagues in solid-cancer patients with hepatic or renal dysfunction [30]. Despite corroborating the results of another trial by failing to show a significant difference in the pharmacokinetics of a 400-mg dose of sorafenib between Child-Pugh A and B patients [31], the authors did find that higher bilirubin concentrations were associated with lower areas under the curve of the main sorafenib metabolite, N-oxidesorafenib, but only in the hepatic and not the renal cohort.…”

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confidence: 99%

Refining Sorafenib Therapy: Lessons from Clinical Practice

et al. 2014

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AbstrAct:Understanding the best use of sorafenib is essential in order to maximize clinical benefit in hepatocellular carcinoma. Based on Phase III and noninterventional study data, as well as our extensive experience, we discuss dose modification in order to manage adverse events, disease response evaluation and how to maximize treatment benefit. Sorafenib should be initiated at the approved dose (400 mg twice daily) and reduced/ interrupted as appropriate in order to manage adverse events. Dose modification should be considered before discontinuation. Appropriate tumor response assessment is critical. Focusing on radiologic response may result in premature sorafenib discontinuation; symptomatic progression should also be considered. If second-line therapies or trials are unavailable, continuing sorafenib beyond radiologic progression may provide a clinical benefit. Our recommendations enable the maximization of treatment duration, and hence clinical benefit, for patients. Keywords:• adverse event managementIt is well established that hepatocellular carcinoma (HCC) is a complex and heterogeneous disease that is affected by multiple genetic and epigenetic alterations [1]. In the overwhelming majority of patients, liver cirrhosis -another complex disease in its own right -is superimposed on HCC. As a result, the prognostic range for these patients varies considerably and continues to change for each patient at every time point over the clinical course of their disease. A meta-analysis of 30 clinical trials into which HCC patients were enrolled for palliative treatment reflects this heterogeneity. It demonstrated a high variability in survival among untreated patients and concluded that no single patient characteristic alone could predict outcome [2].The prognosis and treatment options for HCC are generally related to tumor stage and liver function at presentation [3,4]. In the west, approximately 30% of all patients with HCC are diagnosed in

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confidence: 99%

Refining Sorafenib Therapy: Lessons from Clinical Practice

et al. 2014

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“…Although VEGF-targeted therapies used for mRCC are not renally eliminated, there are some side effects that are more pronounced in patients with renal dysfunction. 44,45 Thus far, no significant pharmacokinetic differences have been observed with VEGF-targeted therapies in the context of renal insufficiency. 35,45,46 A more robust study of patients with severe renal dysfunction (GFR <30 mL/min/1.73 m 2 ) may clarify differences in mRCC patients treated with VEGF-targeted therapies.…”

Section: -419-21mentioning

confidence: 99%

Risk factors and model for predicting toxicity‐related treatment discontinuation in patients with metastatic renal cell carcinoma treated with vascular endothelial growth factor–targeted therapy: Results from the International Metastatic Renal Cell Carcinoma Database Consortium

Kaymakcalan

Xie

Albigès

et al. 2015

Cancer

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BACKGROUND: Vascular endothelial growth factor (VEGF)-targeted therapies are standard treatment for metastatic renal cell carcinoma (mRCC); however, toxicities can lead to drug discontinuation, which can affect patient outcomes. This study was aimed at identifying risk factors for toxicity and constructing the first model to predict toxicity-related treatment discontinuation (TrTD) in mRCC patients treated with VEGF-targeted therapies. METHODS: The baseline characteristics, treatment outcomes, and toxicity data were collected for 936 mRCC patients receiving first-line VEGF-targeted therapy from the International Metastatic Renal Cell Carcinoma Database Consortium. A competing risk regression model was used to identify risk factors for TrTD, and it accounted for other causes as competing risks. RESULTS: Overall, 198 (23.8%) experienced TrTD. Sunitinib was the most common VEGF-targeted therapy (77%), and it was followed by sorafenib (18.4%). The median time on therapy was 7.1 months for all patients and 4.4 months for patients with TrTD. The most common toxicities leading to TrTD included fatigue, diarrhea, and mucositis. In a multivariate analysis, significant predictors for TrTD were a baseline age 60 years, a glomerular filtration rate (GFR) <30 mL/min/1.73 m 2 , a single metastatic site, and a sodium level <135 mmol/L. A risk group model was developed that used the number of patient risk factors to predict the risk of TrTD. CONCLUSIONS: In the largest series to date, age, GFR, number of metastatic sites, and baseline sodium level were found to be independent risk factors for TrTD in mRCC patients receiving VEGF-targeted therapy. Based on the number of risk factors present, a model for predicting TrTD was built to be used as a tool for toxicity monitoring in clinical practice. Cancer 2016;122:411-9.

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“…Sorafenib pharmacokinetics is not altered in patients with moderate hepatic insufficiency (Child-Pugh B status), but these patients are at higher risk of hepatic decompensation and general complications. 9,10 For these patients, a protocol of dose escalation might be adequate to prevent potential complications. 10 While the introduction of sorafenib was a breakthrough in the treatment HCC, its overall efficacy remains modest, with a gain of survival of only a few months.…”

Section: Clinical Use Of Sorafenib In Hccmentioning

confidence: 99%

“…9,10 For these patients, a protocol of dose escalation might be adequate to prevent potential complications. 10 While the introduction of sorafenib was a breakthrough in the treatment HCC, its overall efficacy remains modest, with a gain of survival of only a few months. Furthermore, sorafenib essentially extends the survival of patients with HCC through its ability to slow tumor progression.…”

Section: Clinical Use Of Sorafenib In Hccmentioning

confidence: 99%

Sorafenib and the medical treatment of hepatocellular carcinoma

Galmiche¹,

Chauffer²,

Mazière³

et al. 2011

JST

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Abstract:Hepatocellular carcinoma (HCC) is the most frequent form of primary liver tumor. HCC is characterized by its occurrence in a context of chronic liver disease. The burden of HCC is expected to increase in the coming decade, principally because of its rising incidence. Although radical treatments are available when a unique tumor of small size is found, HCC is more often diagnosed at an advanced stage. Classical schemes for the treatment of advanced HCC have been recently challenged with the introduction of sorafenib (Nexavar . Sorafenib is an inhibitor of oncogenic kinases that has recently been approved as the reference treatment for advanced HCC. Sorafenib affords a modest gain in survival by delaying the progression of HCC. In the absence of validated biomarkers that would predict its efficacy, several questions pertaining to its indications and the follow-up of this treatment remain unanswered. Here, we review the essential facts about sorafenib and its use in HCC. We also put emphasis on the actual research perspectives that could improve HCC treatment based on sorafenib.

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Phase I and Pharmacokinetic Study of Sorafenib in Patients With Hepatic or Renal Dysfunction: CALGB 60301

Cited by 195 publications

References 24 publications

Refining Sorafenib Therapy: Lessons from Clinical Practice

Refining Sorafenib Therapy: Lessons from Clinical Practice

Risk factors and model for predicting toxicity‐related treatment discontinuation in patients with metastatic renal cell carcinoma treated with vascular endothelial growth factor–targeted therapy: Results from the International Metastatic Renal Cell Carcinoma Database Consortium

Sorafenib and the medical treatment of hepatocellular carcinoma

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