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  The first step in inference is prediction of sensitivity val ues for target com

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 The first step in inference is prediction of sensitivity val ues for target com Empty
OdoslaťPredmet: The first step in inference is prediction of sensitivity val ues for target com    The first step in inference is prediction of sensitivity val ues for target com Icon_minitimeŠt apríl 03, 2014 8:27 am

To generate the dynamic model after inhibition of a specific target set S1, we should con sider that the transition i j in the un treated system will be converted to i z in the treated ARN-509 構造 system where z differs from j only in the target set S1 and all targets in S1 have value 0 for z. Each target inhibition combina tion can be considered as multiplying a matrix Tc to the initial transition matrix Q. Each row of Tc contains only one non zero element of 1 based on how the inhibition alters the state. If we consider n targets, n Tcs in combi nation can produce a total of 2n possible transformation matrices T1, T2, T2n. The TIM denotes the state of the LSB of the attractor for the 2n transition matrices T1Q, T2Q, T2nQ starting from initial state 11 1, For instance, if we consider that our drug inhibits the target K3, the discrete dynamic model following application of the drug is shown in Figure 6.<br><br> We should note that the equilibrium AUY922 構造 state of the network 1100 has 0 for the tumor state. This is because the tumor is activated by K3 and inhibition of K3 should eradicate the tumor. On the other hand, since both K1 and K2 can cause tumor through activation of intermediate K3, inhibition of only one of K1 and K2 will not block the tumor. The BN following inhibition of K2 is shown in Figure 7 where the attractor 1011 denotes a tumorous phenotype. Experiment design to infer the dynamic pathway structure The TIM can be used to produce possible dynamic models based on assumptions of latent activa tions or mutations.<br><br> For instance, knowledge of the steady state value of the target K1 following application of target inhibitor for K3, will remove one of the possibilities. Fol lowing inhibition of K3, the value of K1 will remain 1 for the case of Figure 4 as K1 is upstream of K3. Conversely, the value of K1 will be 0 for the second case as K3 activates ALK 阻害剤 K1. In the following paragraphs, we will consider a gen eral pathway obtained from a TIM having the structure shown in Figure 8 but with unknown directionalities of the blocks and target positions. For the current analy sis, we will assume that there are no common targets will be deactivated following the inhibition of block Bi will 1011 be located down stream of Bi. Note that the number of experiments required is based 0111 0110 1010 1110 1111 on steady state measurements following particular per turbations.<br><br> Time series measurements can reduce the 0100 0101 1000 1001 1100 1101 number of experiments required but may not be always technically feasible. In this article, we presented a novel framework for pre dicting the effectiveness of molecularly targeted drugs. We used drug perturbation data to generate a map of the underlying genetic regulatory pathway. Using actual experimental data, we were able to show the effectiveness of our approach for drug sensitivity prediction. The pro posed TIM approach produced a low average leave one out cross validation error of 5% when applied to pertur bation data generated from four primary canine tumors using a set of 60 drugs. We should note that the cur rent 60 drug screen is a small one and technology has been developed for drug screens with a far greater number of drugs.
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