Sentence examples for samples to approximate from inspiring English sources

From the spectral approximation point of view, the problem becomes using M spectral samples to approximate complex sinusoid e j 2 π M mτ up to half a cycle.

The simulation results are obtained by using N s  = N t  = 60 samples to approximate infinite number of samples.

The proposed MSPGF/S can be implemented using cubature [34] and Gauss-Hermite approximations [15], then using respectively L c =2n x =8 and (L_{q} = alpha ^{n_{x}}=81phantom {dot {i}!}) deterministic samples to approximate the integrals of the general solution.

First, the work of Delgado et al. [33] avoided mosaicism by using lymphoid clones, while, second, the study of Ballestar et al. [34] worked with non-subcloned samples to approximate physiological conditions more closely.

Therefore, we propose pre-clustering of input expression samples to approximate condition-specific grouping of samples and individual network construction of each group as a means for dynamic significance thresholding.

As a standard approach, we can use Monte Carlo integration together with the importance sampler to approximate this integral: (12).

Directly calculating (theta) and (phi) was shown to be suboptimal [19], therefore we used a Bayesian approach from the topicmodels package using Gibbs iterative sampling to approximate the distribution z.

This approach begins by assuming a prior distribution on a parameter value of interest, then updates the prior through probabilistic sampling to approximate the posterior distribution on parameter values based on the observed data (Kruschke, 2015).

In the forward pass described in Section 2.1, a set of possible sequences of regimes (a_{1:i-1}^{k}) associated with importance weights (omega _{i-1}^{k}), 1≤k≤N are sampled to approximate p(a i−1,z i−1,z 1:i−1,z

Since the distribution π k over the parameter space after the k-th experiment can not be manipulated analytically, we resort on sampling to approximate it and estimate the integrals by Monte-Carlo simulations.

Primers specific to sequences spanning the junction of exons 50 and 51, present in all DYSF forms, were used to determine the total DYSF mRNA levels, and this served as the 100% DYSF expression value for each sample to approximate the relative expression of the mutant and normal exon 44/45 splice forms.