📄 mbetoolbox_codeml.ctl
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seqfile = abglobin.nuc
treefile =
outfile = mlc * main result file name
noisy = 0 * 0,1,2,3,9: how much rubbish on the screen
verbose = 0 * 0: concise; 1: detailed, 2: too much
runmode = -2 * 0: user tree; 1: semi-automatic; 2: automatic
* 3: StepwiseAddition; (4,5):PerturbationNNI; -2: pairwise
seqtype = 1 * 1:codons; 2:AAs; 3:codons-->AAs
CodonFreq = 3 * 0:1/61 each, 1:F1X4, 2:F3X4, 3:codon table
aaDist = 0 * 0:equal, +:geometric; -:linear, 1-6:G1974,Miyata,c,p,v,a
model = 0 * 0:one, 1:b, 2:2 or more dN/dS ratios for branches
NSsites = 0 * 0:one w;1:neutral;2:selection; 3:discrete;4:freqs;
* 5:gamma;6:2gamma;7:beta;8:beta&w;9:betaγ
* 10:beta&gamma+1; 11:beta&normal>1; 12:0&2normal>1;
* 13:3normal>0
icode = 0 * 0:universal code; 1:mammalian mt; 2-10:see below
Mgene = 0 * 0:rates, 1:separate; 2:diff pi, 3:diff kapa, 4:all diff
fix_kappa = 0 * 1: kappa fixed, 0: kappa to be estimated
kappa = 2 * initial or fixed kappa
fix_omega = 0 * 1: omega or omega_1 fixed, 0: estimate
omega = 3.14159 * initial or fixed omega, for codons
fix_alpha = 1 * 0: estimate gamma shape parameter; 1: fix it at alpha
alpha = 0. * initial or fixed alpha, 0:infinity (constant rate)
Malpha = 0 * different alphas for genes
ncatG = 2 * # of categories in dG of NSsites models
clock = 0 * 0:no clock, 1:global clock; 2:local clock; 3:TipDate
getSE = 0 * 0: don't want them, 1: want S.E.s of estimates
RateAncestor = 0 * (0,1,2): rates (alpha>0) or ancestral states (1 or 2)
* Genetic codes: 0:universal, 1:mammalian mt., 2:yeast mt., 3:mold mt.,
* 4: invertebrate mt., 5: ciliate nuclear, 6: echinoderm mt.,
* 7: euplotid mt., 8: alternative yeast nu. 9: ascidian mt.,
* 10: blepharisma nu.
* These codes correspond to transl_table 1 to 11 of GENEBANK.
Small_Diff = .5e-6
* cleandata = 1 * remove sites with ambiguity data (1:yes, 0:no)?
* ndata = 2
* fix_blength = -1 * 0: ignore, -1: random, 1: initial, 2: fixed
method = 1 * 0: simultaneous; 1: one branch at a time
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