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1.
Semiparametric models for cumulative incidence functions   总被引:1,自引:0,他引:1  
Bryant J  Dignam JJ 《Biometrics》2004,60(1):182-190
In analyses of time-to-failure data with competing risks, cumulative incidence functions may be used to estimate the time-dependent cumulative probability of failure due to specific causes. These functions are commonly estimated using nonparametric methods, but in cases where events due to the cause of primary interest are infrequent relative to other modes of failure, nonparametric methods may result in rather imprecise estimates for the corresponding subdistribution. In such cases, it may be possible to model the cause-specific hazard of primary interest parametrically, while accounting for the other modes of failure using nonparametric estimators. The cumulative incidence estimators so obtained are simple to compute and are considerably more efficient than the usual nonparametric estimator, particularly with regard to interpolation of cumulative incidence at early or intermediate time points within the range of data used to fit the function. More surprisingly, they are often nearly as efficient as fully parametric estimators. We illustrate the utility of this approach in the analysis of patients treated for early stage breast cancer.  相似文献   

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Motivated by a study on pregnancy outcome, a computationally simple resampling procedure for nonparametric analysis of the cumulative incidence function of a competing risk is investigated for left‐truncated data. We also modify the original procedure to producing the more desirable Greenwood‐type variance estimates. These approaches are used to construct simultaneous confidence bands of the cumulative incidence functions which is otherwise hampered by the complicated nature of the covariance process. Simulation results and a real data example are provided.  相似文献   

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We develop time‐varying association analyses for onset ages of two lung infections to address the statistical challenges in utilizing registry data where onset ages are left‐truncated by ages of entry and competing‐risk censored by deaths. Two types of association estimators are proposed based on conditional cause‐specific hazard function and cumulative incidence function that are adapted from unconditional quantities to handle left truncation. Asymptotic properties of the estimators are established by using the empirical process techniques. Our simulation study shows that the estimators perform well with moderate sample sizes. We apply our methods to the Cystic Fibrosis Foundation Registry data to study the relationship between onset ages of Pseudomonas aeruginosa and Staphylococcus aureus infections.  相似文献   

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