mgltools 1.5.7
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Theta Regija

THETA REGIJA

KNJIGA – Theta isceljivanje (HR)
mgltools 1.5.7

THETA REGIJA

1.5.7 | Mgltools

U ovoj knjizi autorica Vianna Stibal otkriva jednu od najmoćnijih tehnika energetskog iscjeljivanja ikad izloženu u pisanom tekstu: Theta iscjeljivanje.

  • Autor: Vianna Stibal
  • Format: 24 x 15,5 cm; 316 str., meki uvez, šivano
  • Jezik: Prevod na HR jezik
25,00 €

Plačilo naročila

UMIRJEN UM, Boštjan Cvetič s.p., izobraževanje in svetovanje
Nasipna ulica 5 2234 Benedikt Slovenija

IBAN SI56 0400 0028 1290 338
BIC (SWIFT) KODA: KBMASI2X

1.5.7 | Mgltools

KNJIGA – Theta isceljivanje (HR)

Theta iscjeljivanje je meditativni proces koji donosi fizičko, psihološko i duhovno iscjeljenje kroz usredotočenu molitvu Stvoritelju. Ova knjiga je spoj prošlih djela Idi gore i traži Boga, Idi gore i radi s Bogom, Priručnika za Napredni DNK2 tečaj kao i novih informacija koje su se razvile otkako su ta tri djela napisana. Knjiga sadrži 32 poglavlja u kojima su prikazane tehnike intuitivnog očitavanja i iscjeljivanja, rada na vjerovanjima i osjećajima, DNK aktivacije, zamjene gene i još mnogo toga potkrijepljeno primjerima iz stvarne prakse. Pojašnjeni su sedam nivoa postojanja koji pružaju uvid u razumijevanje kako i zašto svijet djeluje na tjelesnim i duhovnim razinama, te kako se to odnosi na čovjeka. Jedan dio knjige posvećen je razvoju Djece novog doba te s kakvom se vrstom izazova i problema ta djeca susreću u mladoj dobi. Knjiga donosi i svjedočanstva onih kojima je Theta iscjeljivanje uistinu promijenilo život. Postupci Theta iscjeljivanja nisu ograničeni ni za jednu dob, spol, rasu, boju kože, vjeru ili religiju. Svatko tko ima čistu vjeru u Boga ili u Stvaralačku energiju može koristiti ovu tehniku.

Kontakti za naročilo

SLOVENIJA i(n) CELOTNA REGIJA 
  • Informacije
  • E-pošta
  • Tel
  • Informacije, naročila, prevzem knjig – LJUBLJANA, MARIBOR
  • info@umirjenum.si
  • (+386) 68 633 738 (Boštjan)
HRVATSKA
  • Informacije
  • E-pošta
  • Tel
  • Narudžbe, preuzimanje knjiga – ZAGREB
  • thetaregijazg@gmail.com
  • (+385) 97 662 1334 (Ga. Tea)
SRBIJA
  • Informacije
  • E-pošta
  • Tel
  • Porudžbine, preuzimanje knjiga – BEOGRAD
  • thetaregijabg@gmail.com
  • (+381) 69 222 6056 (Ga. Olgica)

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1.5.7 | Mgltools

The enduring legacy of MGLTools 1.5.7 is its role as a . By providing a free, cross-platform (Windows, macOS, Linux) interface to high-end docking algorithms, it empowered undergraduate students, small labs, and researchers in developing nations to participate in drug discovery. Many of today’s computational chemists first learned the steps of docking—from cleaning a protein to analyzing a cluster of binding poses—using this very version. It transformed molecular docking from a black art into a reproducible, teachable workflow.

Another hallmark of version 1.5.7 is its handling of . While docking typically treats the protein as rigid for computational speed, key side chains (e.g., in an enzyme’s active site) can move upon ligand binding. MGLTools 1.5.7 allows users to define which residues should be flexible, generating separate PDBQT files for the rigid backbone and the mobile side chains. This feature, now standard, was a significant step toward more realistic induced-fit modeling. Additionally, the software includes AutoGrid utilities to pre-calculate interaction energy maps, dramatically accelerating the subsequent docking search. mgltools 1.5.7

In conclusion, MGLTools 1.5.7 is far more than a piece of deprecated software; it is a historical artifact and a functional workhorse. It captures a pivotal moment when computational biology matured from command-line hacking to structured science. While newer, sleeker tools have emerged, the principles embedded in MGLTools 1.5.7—meticulous preparation, transparent file formats, and modular design—remain the gold standard. For anyone seeking to understand how a computer "sees" a protein or how a potential drug first finds its target, MGLTools 1.5.7 serves as both a practical instrument and a digital lens, revealing the hidden choreography of the molecular world. The enduring legacy of MGLTools 1

However, no scientific tool is without limitations, and MGLTools 1.5.7 is a product of its time. Its interface, built on the legacy Tkinter and OpenGL libraries, feels distinctly early-2000s: menus are dense, the rendering engine is basic compared to modern tools like PyMOL or ChimeraX, and it is prone to crashes when handling very large complexes (e.g., ribosomes or multi-protein assemblies). Moreover, it requires a functional Python 2.7 environment—a version now long deprecated—making installation on modern operating systems increasingly reliant on virtual machines or containers. Yet, paradoxically, this "aging" quality is also a form of stability; the workflow has remained unchanged for years, ensuring that protocols and tutorials from 2015 remain perfectly valid today. It transformed molecular docking from a black art

In the computational study of biomolecular interactions, the adage "garbage in, garbage out" holds absolute authority. Before a powerful program like AutoDock can predict how a drug candidate binds to a cancer protein, the raw data of a protein structure must be translated into a language computers can understand. For over a decade, one software suite has served as the essential bridge between the chaotic world of experimental biology and the pristine logic of simulation: MGLTools (Molecular Graphics Laboratory Tools) . Version 1.5.7 represents a mature, stable, and historically critical release of this indispensable toolkit, embodying the principles of accessibility, utility, and scientific rigor that have democratized molecular docking.

The true genius of MGLTools 1.5.7 lies in its handling of , a deceptively complex task. Raw protein structures from the Protein Data Bank (PDB) often contain only heavy atoms, lack hydrogen atoms (critical for hydrogen bonding simulations), and include water molecules or co-factors that may or may not be relevant to docking. MGLTools 1.5.7 automates the tedious but vital process of adding hydrogens, computing Gasteiger charges, merging non-polar hydrogens, and detecting aromatic carbons. Furthermore, it introduces the concept of "docking-ready" PDBQT files —an extension of the PDB format that includes partial charges (Q) and atom types (T) recognized by AutoDock’s empirical free energy force field. Without MGLTools, manually formatting a PDBQT file for a 300-residue protein would be a recipe for human error.

At its core, MGLTools 1.5.7 is not a docking engine itself but a for the AutoDock family of software (AutoDock4 and AutoDock Vina). Released during a period when computational chemistry was shifting from command-line exclusivity to user-friendly applications, version 1.5.7 consolidated essential functionalities into a cohesive environment. It includes three primary components: Python Molecular Viewer (PMV) for visualization, AutoDockTools (ADT) for preparing docking input files, and Vision for building Python-based scientific applications. This modular architecture allows researchers to inspect a protein, add missing atoms, assign partial charges, detect rotatable bonds, and define binding sites—all within a single, unified workspace.