Protein Binding: Difference between revisions

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This module can be used to predict plasma protein bound fraction and the equilibrium binding constant to serum albumin of a compound. The binding properties are computed from physicochemical properties (lipophilicity, ionization constants, hydrogen bonding capacity) and structural descriptors of the compounds. Reliability of each prediction is assessed by calculating corresponding Reliability Indices (see [[Trainable_Models#Overview|Overview of the Trainable models]]).
This module can be used to predict plasma protein bound fraction and the equilibrium binding constant to serum albumin of a compound. The binding properties are computed from lipophilicity and structural descriptors of the compounds. Reliability of each prediction is assessed by calculating corresponding Reliability Indices.
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* Main plasma proteins that mostly contribute to binding of different compound classes in human plasma are enumerated in the textual comments next to the prediction results.
* Main plasma proteins that mostly contribute to binding of different compound classes in human plasma are enumerated in the textual comments next to the prediction results.
* Experimentally measured extent of plasma protein binding, human serum albumin affinity constants are displayed for up to 5 similar structures from the training set along with the corresponding literature references.
* Experimentally measured extent of plasma protein binding, human serum albumin affinity constants are displayed for up to 5 similar structures from the training set along with the corresponding literature references.
* A clear and straightforward interface ensures quick and easy addition of user-defined data to the Self-training Library.
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<span style="color:red; font-weight: bold;">IMPORTANT NOTE:</span>
If you installed Percepta as an upgrade over a previous version, the program will attempt to preserve any custom configuration of Self-training libraries used in Protein Binding module. This configuration will not include the new, significantly extended built-in library that was introduced in 2024 release. In this case, to take advantage of the new library, you may need to click "Configure" and manually select the following entry: ''%PPB v. 1.3 (read-only)''.
In case of a new installation, the new library should be selected automatically with no further action required.


== Interface ==
== Interface ==
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# Calculated plasma protein bound fraction and logarithm of the affinity constant to human serum albumin in the blood plasma:<br>[[File:distribution_ppb_scale.png|500px]]
# Calculated plasma protein bound fraction and logarithm of the affinity constant to human serum albumin in the blood plasma:<br>[[File:Distribution_ppb_scale.png|500px]]
# Reliability indices of predictions are provided along with the calculated values
# Reliability indices of predictions are provided along with the calculated values. Each of the properties also has dedicated "Configure" and "Train" buttons to select the training library for use in calculations and to add new data to that library. The name of the currently selected library is indicated with italic font.
# A brief general description of a compound’s likely binding behavior when dissolved in blood plasma, based on its physicochemical properties
# A brief general description of a compound’s likely binding behavior when dissolved in blood plasma, based on its physicochemical properties
# Each of the properties has dedicated "Configure" and "Train" buttons to select the training library for use in calculations and to add new data to that library
# Up to 5 similar structures in the protein binding training set with experimental quantitative values of %PPB, LogK<sub>a</sub><sup>HSA</sup> and literature references
# Up to 5 similar structures in the protein binding training set with experimental quantitative values of %PPB, LogK<sub>a</sub><sup>HSA</sup> and literature references
# Switch between tabs displaying similar structures from %PPB and LogK<sub>a</sub><sup>HSA</sup> databases
# Switch between tabs displaying similar structures from %PPB and LogK<sub>a</sub><sup>HSA</sup> databases
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==Technical information==
==Technical information==
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* %PPB values represent the overall fraction of drug bound in human plasma, i.e. accounts for interactions with different proteins: albumin, alpha<sub>1</sub>-acid glycoprotein, lipoproteins, SHBG, transcortin etc. ''In vitro'' measurements of the extent of plasma protein binding usually involve equilibrium dialysis, ultrafiltration or ultracentrifugation methods.
* %PPB values represent the overall fraction of drug bound in human plasma, i.e. accounts for interactions with different proteins: albumin, alpha<sub>1</sub>-acid glycoprotein, lipoproteins, SHBG, transcortin etc. ''In vitro'' measurements of the extent of plasma protein binding usually involve equilibrium dialysis, ultrafiltration or ultracentrifugation methods.
%PPB = (1 – ''f<sub>u</sub>'') * 100% where ''f<sub>u</sub>'' is fraction of free (unbound) drug in plasma ranging from 0 to 1.
%PPB = (1 – ''f<sub>u</sub>'') * 100% where ''f<sub>u</sub>'' is fraction of free (unbound) drug in plasma ranging from 0 to 1.
* Supplementary Distribution\Vd module calculates apparent Volume of Distribution of drugs in human body expressed in liters per kg body weight (L/kg).
* Distribution\Vd module calculates apparent Volume of Distribution of drugs in human body expressed in liters per kg body weight (L/kg).


===Experimental data===
===Experimental data===
Experimental data that were utilized to build predictive models were collected from drug prescription information, reference pharmacokinetic tabulations and many original articles. The main sources of Vd data were well-known pharmacokinetic books: "Therapeutic Drugs" (ed. by C. dollery), and Goodman & Gilman's "The Pharmacological Basis of Therapeutics", while albumin affinity constants were collected mainly from original articles by Valko K. et al. ''J Pharm Sci.'' '''2003''';92(11):2236-48. [http://www3.interscience.wiley.com/journal/104556357/abstract], and Kratochwil N.A. et al. ''Biochem Pharmacol.'' '''2002''';64(9):1355-74. [http://www.sciencedirect.com/science?_ob=ArticleURL&_udi=B6T4P-461XRMC-1&_user=10&_rdoc=1&_fmt=&_orig=search&_sort=d&view=c&_acct=C000050221&_version=1&_urlVersion=0&_userid=10&md5=290e081e0775f2be854e4e503160ba2a]
Experimental data that were utilized to build predictive models were collected from drug prescription information, reference pharmacokinetic tabulations and many original articles. The main sources of Vd data were well-known pharmacokinetic books: "Therapeutic Drugs" (ed. by C. dollery), and Goodman & Gilman's "The Pharmacological Basis of Therapeutics", while albumin affinity constants were collected mainly from original articles by Valko K. et al. ''J Pharm Sci.'' '''2003''';92(11):2236-48. [https://pubmed.ncbi.nlm.nih.gov/14603509], and Kratochwil N.A. et al. ''Biochem Pharmacol.'' '''2002''';64(9):1355-74. [https://pubmed.ncbi.nlm.nih.gov/12392818]
The compiled data sets contain %PPB data for almost 1500 compounds, about 340 albumin affinity constants and almost 800 Vd values.
The compiled data sets contain %PPB data for almost 1500 compounds, about 340 albumin affinity constants and almost 800 Vd values.


===Model development (technical details)===
===Model development (technical details)===
The models for predicting %PPB and log ''K<sub>a</sub><sup>HSA</sup>'' constants were developed with Algorithm Builder using a novel methodology consisting of two parts:
* Global baseline statistical model employing binomial PLS with multiple bootstrapping using a predefined set of fragmental descriptors.
* Local correction to baseline prediction based on analysis of experimental data for similar compounds.
The underlying methodology enables obtaining an intrinsic evaluation of prediction confidence by the means of Reliability Index (RI) values calculated for each prediction. RI ranging from 0 to 1 serves as an indication whether a submitted compound falls within the Model Applicability Domain. Two criteria influence the calculation od Reliability Index of a prediction:
* Similarity of the analyzed molecule to compounds in the Self-training Library (prediction is unreliable if no similar compounds have been found in the Library).
* Consistency of experimental data for similar compounds – reliability of calculated values is lower is data for similar compounds are discrepant.


Both %PPB and log ''K<sub>a</sub><sup>HSA</sup>'' predictive models are '''Trainable''' meaning that their Applicability Domains may be easily extended by addition of ‘in-house’ experimental data to the module Self-training Library. Notably, the baseline statistical model does not need to be rebuilt from scratch to account for data entered by the user. The model is retrained automatically as new compounds are added to the Library. Model trainability would be particularly useful for predicting serum albumin affinity constants as literature data sets are very sparse, thus the ability to take advantage of large ‘in-house’ libraries gives the potential for a significant improvement of both accuracy and reliability of calculations.
The predictive models of %PPB and log ''K<sub>a</sub><sup>HSA</sup>'' were derived using GALAS (Global, Adjusted Locally According to Similarity) modeling methodology (please refer to [http://www.ncbi.nlm.nih.gov/pubmed/20373217] for more details).
 
Each GALAS model consists of two parts:
* Global (baseline) statistical model that reflects general trends in the variation of the property of interest.
* Similarity-based routine that performs local correction of baseline predictions taking into account the differences between baseline and experimental values for the most similar training set compounds.
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GALAS methodology also provides the basis for estimating reliability of predictions by the means of calculated Reliability Index (''RI'') value that takes into account:
* Similarity of tested compound to the training set molecules.
* Consistence of experimental values and baseline model prediction for the most similar similar compounds from the training set.
 
Reliability Index ranges from 0 to 1 (0 corresponds to a completely unreliable, and 1 - a highly reliable prediction) and serves as an indication whether a submitted compound falls within the Model Applicability Domain. Compounds obtaining predictions ''RI'' < 0.3 are considered outside of the Applicability Domain of the model.
 
Both %PPB and log ''K<sub>a</sub><sup>HSA</sup>'' are '''Trainable''' meaning that their Applicability Domains may be easily extended by addition of ‘in-house’ experimental data to the module Self-training Library. Notably, the baseline statistical model does not need to be rebuilt from scratch to account for data entered by the user. The model is retrained automatically as new compounds are added to the Library. Model trainability would be particularly useful for predicting serum albumin affinity constants as literature data sets are very sparse, thus the ability to take advantage of large ‘in-house’ libraries gives the potential for a significant improvement of both accuracy and reliability of calculations.
 
Volume of Distribution uses a mechanistic model based on physiological Øie-Tozer equation that relates Vd to the fraction unbound in plasma (calculated using %PPB model described above) and fraction unbound in tissues (calculated by a non-linear ionization-specific model in terms of LogP and pKa). For more technical details about %PPB and Vd models please refer to [http://perceptahelp.acdlabs.com/docs/Distribution.pdf].
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Latest revision as of 07:29, 24 September 2024

Overview


This module can be used to predict plasma protein bound fraction and the equilibrium binding constant to serum albumin of a compound. The binding properties are computed from lipophilicity and structural descriptors of the compounds. Reliability of each prediction is assessed by calculating corresponding Reliability Indices.

Features

  • Calculates %PPB – the cumulative percentage of the analyzed compound bound to human plasma proteins (such as albumin, alpha1-acid glycoprotein and others) and log KaHSA – human serum albumin affinity constants. with Reliability Index (RI) values of the corresponding predictions.
  • RI values represent a quantitative evaluation of prediction confidence. High RI shows that the calculated value is likely to be accurate, while low RI indicates that no similar compounds with consistent data are present in the training set.
  • Main plasma proteins that mostly contribute to binding of different compound classes in human plasma are enumerated in the textual comments next to the prediction results.
  • Experimentally measured extent of plasma protein binding, human serum albumin affinity constants are displayed for up to 5 similar structures from the training set along with the corresponding literature references.


IMPORTANT NOTE:

If you installed Percepta as an upgrade over a previous version, the program will attempt to preserve any custom configuration of Self-training libraries used in Protein Binding module. This configuration will not include the new, significantly extended built-in library that was introduced in 2024 release. In this case, to take advantage of the new library, you may need to click "Configure" and manually select the following entry: %PPB v. 1.3 (read-only).

In case of a new installation, the new library should be selected automatically with no further action required.

Interface


Distribution ppb.png


  1. Calculated plasma protein bound fraction and logarithm of the affinity constant to human serum albumin in the blood plasma:
    Distribution ppb scale.png
  2. Reliability indices of predictions are provided along with the calculated values. Each of the properties also has dedicated "Configure" and "Train" buttons to select the training library for use in calculations and to add new data to that library. The name of the currently selected library is indicated with italic font.
  3. A brief general description of a compound’s likely binding behavior when dissolved in blood plasma, based on its physicochemical properties
  4. Up to 5 similar structures in the protein binding training set with experimental quantitative values of %PPB, LogKaHSA and literature references
  5. Switch between tabs displaying similar structures from %PPB and LogKaHSA databases

Note: Prediction reliability classification according to Reliability Index (RI) values:

  • RI < 0.3 – Not Reliable,
  • RI in range 0.3-0.5 – Bordeline Reliability,
  • RI in range 0.5-0.75 – Moderate Reliability,
  • RI >= 0.75 – High Reliability



Technical information


Calculated quantitative parameters

Parameters calculated by Distribution\Protein Binding module include percentage plasma protein binding values (%PPB) and log KaHSA constants. These properties are related, but characterize provide slightly different information about the considered process.

  • log KaHSA represents the drug’s affinity constant to human serum albumin – the major carrier protein in plasma. Experimental data come from direct chromatographic determination of binding strength to that particular protein.

log KaHSA = log ([LA]/([L][A])) where [LA] is concentration of ligand bound to albumin, [L] – that of free ligand, and [A] – concentration of free albumin which is estimated at ~0.6 mM in human plasma.

  • %PPB values represent the overall fraction of drug bound in human plasma, i.e. accounts for interactions with different proteins: albumin, alpha1-acid glycoprotein, lipoproteins, SHBG, transcortin etc. In vitro measurements of the extent of plasma protein binding usually involve equilibrium dialysis, ultrafiltration or ultracentrifugation methods.

%PPB = (1 – fu) * 100% where fu is fraction of free (unbound) drug in plasma ranging from 0 to 1.

  • Distribution\Vd module calculates apparent Volume of Distribution of drugs in human body expressed in liters per kg body weight (L/kg).

Experimental data

Experimental data that were utilized to build predictive models were collected from drug prescription information, reference pharmacokinetic tabulations and many original articles. The main sources of Vd data were well-known pharmacokinetic books: "Therapeutic Drugs" (ed. by C. dollery), and Goodman & Gilman's "The Pharmacological Basis of Therapeutics", while albumin affinity constants were collected mainly from original articles by Valko K. et al. J Pharm Sci. 2003;92(11):2236-48. [1], and Kratochwil N.A. et al. Biochem Pharmacol. 2002;64(9):1355-74. [2] The compiled data sets contain %PPB data for almost 1500 compounds, about 340 albumin affinity constants and almost 800 Vd values.

Model development (technical details)

The predictive models of %PPB and log KaHSA were derived using GALAS (Global, Adjusted Locally According to Similarity) modeling methodology (please refer to [3] for more details).

Each GALAS model consists of two parts:

  • Global (baseline) statistical model that reflects general trends in the variation of the property of interest.
  • Similarity-based routine that performs local correction of baseline predictions taking into account the differences between baseline and experimental values for the most similar training set compounds.


GALAS methodology also provides the basis for estimating reliability of predictions by the means of calculated Reliability Index (RI) value that takes into account:

  • Similarity of tested compound to the training set molecules.
  • Consistence of experimental values and baseline model prediction for the most similar similar compounds from the training set.

Reliability Index ranges from 0 to 1 (0 corresponds to a completely unreliable, and 1 - a highly reliable prediction) and serves as an indication whether a submitted compound falls within the Model Applicability Domain. Compounds obtaining predictions RI < 0.3 are considered outside of the Applicability Domain of the model.

Both %PPB and log KaHSA are Trainable meaning that their Applicability Domains may be easily extended by addition of ‘in-house’ experimental data to the module Self-training Library. Notably, the baseline statistical model does not need to be rebuilt from scratch to account for data entered by the user. The model is retrained automatically as new compounds are added to the Library. Model trainability would be particularly useful for predicting serum albumin affinity constants as literature data sets are very sparse, thus the ability to take advantage of large ‘in-house’ libraries gives the potential for a significant improvement of both accuracy and reliability of calculations.

Volume of Distribution uses a mechanistic model based on physiological Øie-Tozer equation that relates Vd to the fraction unbound in plasma (calculated using %PPB model described above) and fraction unbound in tissues (calculated by a non-linear ionization-specific model in terms of LogP and pKa). For more technical details about %PPB and Vd models please refer to [4].

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