Robert E. Dorsey scite author profile

JSTOR is a not-for-profit service that helps scholars, researchers, and students discover, use, and build upon a wide range of content in a trusted digital archive. We use information technology and tools to increase productivity and facilitate new forms of scholarship. For more information about JSTOR, please contact support@jstor.org.. American Statistical Association is collaborating with JSTOR to digitize, preserve and extend access to Journal of Business &Economic Statistics.The genetic algorithm is examined as a method for solving optimization problems in econometric estimation. It does not restrict either the form or regularity of the objective function, allows a reasonably large parameter space, and does not rely on a point-to-point search. The performance is evaluated through two sets of experiments on standard test problems as well as econometric problems from the literature. First, alternative genetic algorithms that vary over mutation and crossover rates, population sizes, and other features are contrasted. Second, the genetic algorithm is compared to Nelder-Mead simplex, simulated annealing, adaptive random search, and MSCORE.

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Optimization of neural networks: A comparative analysis of the genetic algorithm and simulated annealing

Sexton¹,

Dorsey²,

Johnson³

1999

European Journal of Operational Research

194

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Expression Patterns of Retinoblastoma Protein in Parkinson Disease

Jordan‐Sciutto

Dorsey

Chalovich

et al. 2003

J Neuropathol Exp Neurol

112

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Cellular mechanisms implicated in Parkinson disease (PD) include oxidative stress, inflammatory response, excess dopamine, DNA damage, and loss of trophic support. These stimuli have been observed to induce changes in cell cycle proteins in several cell types. One of the key regulators of cell cycle progression is the retinoblastoma protein (pRb); therefore, we assessed the staining for pRb and its inactive hyperphosphorylated isoform, ppRb, in autopsy tissue from patients with PD. In PD we found abundant pRb staining in neuronal cytoplasm of the substantia nigra, mid-frontal cortex, and hippocampus by immunohistochemistry. In controls, pRb weakly stained nucleoli of neurons in the substantia nigra and exhibited no detectable staining in mid-frontal cortex and hippocampus. Staining for ppRb resulted in a shift from weak cytoplasmic staining in neurons from control cases to strong nuclear staining in PD cases, especially within the substantia nigra, mid-frontal cortex, and hippocampus. In the substantia nigra, ppRb also co-localized to Lewy bodies, which are a pathologic feature of PD. Lewy bodies are also found in diffuse Lewy body disease (DLBD) that do not consistently exhibit changes in pRb or ppRb. These results indicate that there are changes in pRb and its inactive phospho-isoform in neurons responding to neurodegenerative stimuli associated with PD.

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Robert E. Dorsey

Toward global optimization of neural networks: A comparison of the genetic algorithm and backpropagation

Genetic Algorithms for Estimation Problems with Multiple Optima, Nondifferentiability, and Other Irregular Features

Optimization of neural networks: A comparative analysis of the genetic algorithm and simulated annealing

Expression Patterns of Retinoblastoma Protein in Parkinson Disease

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