Monday, October 14, 2019
Dipole Moment of 5- Fluorouracil Molecule
Dipole Moment of 5- Fluorouracil Molecule Computational Term Paper: Theoretical studies on 5- fluorouracil to calculate its dipole moment, and how the values compare with other pyrimidine analog (namely uracil and thymine) and that of literature. Name: Farzana Nushin Rezvi Abstract: In this experiment, the dipole moment of 5- Fluorouracil molecule was determined using the Gaussian software, and compared with literature values. The dipole moments of other pyrimidine analogs, namely Thymine and Uracil, were also calculated and compared with literature values. The experiment gave insight to typical dipole moment values of uracil derivatives, and how the dipole moment of aromatic molecules can be influenced in the presence of ââ¬âF, or -CH3 substituent. Introduction: The purpose of this experiment is to calculate the dipole moment of the anticancer drug, 5- Fluorouracil, and compare the numerical value with that of two other pyrimidines, Thymine and Uracil. Fig 1: Molecular structure of 5- Fluoro uracil (drawn by ChemBioDraw). 5- Fluorouracil is apyrimidine analog (nucleoside analogs that mimic the molecular structure of pyrimidines) of uracil molecule that functions as an anti-cancer drug; it is used in the treatment of several types of cancer, including that of rectum, colon, head and neck cancer.10 5- Fluorouracil belongs to the family of drugs called theantimetabolites. Antimetabolite drugs function by impeding vital biosynthetic processes or by being assimilated into macromolecules, and inhibiting their normal functioning. The fluoro pyrimidine drug, 5-fluorouracil (5-FU) does both.9Cancer cells often use more uracil than normal cells, which indicates that uracil metabolism is a potential target for antimetabolite chemotherapy.9 ââ¬Å"The mechanism of cytotoxicity of 5-FU has been ascribed to the misincorporation of fluoronucleotides into RNA and DNA and to the inhibition of the nucleotide synthetic enzyme thymidylate synthase.â⬠9 Thymidylate synthase is an enzyme that catalyzes the conversion o f deoxyuridine monophosphate (dUMP) to deoxythymidine monophosphate (dTMP). dTMP is one of the three nucleotides (dTMP, dTTP, and dTDP) that eventually produce a thymine molecule. With inhibition of Thymidylate synthase, an imbalance of nucleotides results and increased levels of dUTP arise. Both of these factors cause DNA damage, therefore ultimately inhibiting cell replication. 5 FU is also seldom found in skin creams used for other conditions. However, it should be used in moderate/regulated amounts since the side effects of unregulated exposure can be severe.10 5-Fluorouracil is a derivative of Uracil. Another structural analog of Uracil is Thymine. As can be seen from the figure below, the molecules only differ in what substituent each has on C-5. Fig 2: Molecular structures of Uracil, 5-Fluorouracil, and Thymine. Thymine is one of the four nucleobases of DNA. Uracil is the RNA analogue of Thymine. Unlike Fluorouracil, these bases are regularly used by a healthy cell to construct new nucleotides (for multiplication, repair, etc.) The dipole moment is considered to be an elementary physiochemical property of a molecule. Interpretation of dipole moments by electronic charge distribution contributes to the understanding the molecular electronic structure and helps us gain deeper insight. The numerical values of the dipole moments also help us in evaluating the quantum mechanical calculations of electronic charge distribution, particularly in a series of homologous compounds, as in our experiment. Our experiment helps us understand the effects of substituents at C5 dipole moment of uracil. The dipole moment is a of these three molecules is an interesting study because in each case, the dipole moment is primarily influenced by the presence of electronegative atoms. The dipole moment of a molecule influences many of its properties and features (such as its colligtaive properties, how it interacts with other molecules, its behavior in compounds, etc.) In the molecules under consideration, the dipole moment(s) work as in the following figure (the dipole moment of uracil directed inbetween N3 and C4, with the substituent ââ¬ËXââ¬â¢ either strengthening, or weakening the dipole in the illustrated vectors)6: Fig 3: Vector scheme of dipole moments in uracil and in its derivatives6 (reproduced using ChemBioDraw) Experimental: For this Lab, the Gaussian software was used in calculating the dipole moment. At first, the molecule of concern was drawn using the software. Then ââ¬ËEditââ¬â¢ option is selected to ââ¬ËSymmetrizeââ¬â¢ our subject molecule. After that is done, we perform Gaussian Calculation Setup, by selecting Job Type as ââ¬ËEnergyââ¬â¢, and under Methods changing the Basis set. The numerical value of the dipole moment is obtained from the ââ¬ËResultsââ¬â¢ of the .chk file. The Gaussian calculation is repeated by selecting other Basis sets. The whole process is repeated for the molecules Thymine and Uracil. The molecule is drawn using Gaussian, and the Gaussian calculations repeated by selecting different ââ¬Ëjob typesââ¬â¢ and ââ¬Ëbasis setsââ¬â¢. Results: The results obtained are represented in tabular form. The screenshots of the molecules as drawn in the Gaussian software are also given. Tables: Table 1: The theoretical and Literature values of 5-Fluorouracil dipole moment Table 2: The theoretical and Literature values of Uracil dipole moment Table 3: The theoretical and Literature values of Thymine dipole moment. Images obtained from Gaussian: 5-Fluorouracil Fig 4: Image of 5-Fluorouracil molecule as drawn using Gaussian software Uracil: Fig 5: Image of uracil molecule as drawn using Gaussian software Thymine: Fig 6: Image of thymine molecule as drawn using Gaussian software Discussion: The purpose of this experiment was to calculate the numerical values of dipole moments of the anticancer drug, 5- fluorouracil, and two other pyrimidines, thymine and uracil, and compare the obtained values with that of literature values. The dipole moment of a bond is defined as the mathematical product of the magnitude of the charges and distance between atoms under consideration11. The numerical value of the dipole moment can be calculated for each bond, as well as for the entire molecule. In this experiment, we use the Gaussian software for the calculation of dipole moments. The calculation of dipole moment is based on the allocation of atomic charges to the atoms in the molecule in a reasonable way.4 In the hands on experiment, this consists of assigning electronegativity values to the atoms and experimental structural information of the bonds. Topological methods, however, do not take in information about the molecular geometry or the conformational status of the molecule. The topological method currently in use is the Gasteiger-Hà ¼ckelmethod, which has the disadvantage of omitting the validation procedure. This renders the study impractical.11 The method of computation of partial charges employed in this experiment is based on the quantum mechanical calculation of wavefunction.11 For this report, wavefunctions were obtained using the ab initio method. Ab initio means based on first principles, these methods are based on quantum mechanics and attempt to solve the Schrà ¶dinger equation. ââ¬Å"Ab initio methods use no experimental parameters in their calculations, although they use some mathematical approximations. The major disadvantage of Ab Initio quantum chemistry is the heavy demands on computer power.â⬠12 The choice of basis set is one of the most important aspects of this computation, as our results depend vastly on the basis set employed. Basis sets are quantum chemical units of energy; basis set contains mathematical functions that can be used to determine the dipole moment, energy, and other quantum mechanical properties of an atom/molecule of study. Basis sets are considered to represent the wavefunctions of the electrons in the species.12 On the basis of atomic point charges, a molecular dipole moment can be calculated in a quite simple and fast way, and compared with literature values. To get reliable results using this method, one must select small and rigid structures.11 As the dipole moment is a property defined by quantum mechanics, wavefunctions can be used to directly calculate its values. Results derived with large basis sets (such as those reported in this paper) are in good agreement with experimental values. As we can see, our calculated values of the dipole moment align quite closely with the experimental values. One fact, however, stands out: the values of dipole moment get closer to the ââ¬Ëliterature valuesââ¬â¢ as the basis set is increased. However, quantum mechanical methods are not very useful when obtaining information about larger molecules.11 The dipole moments of uracil, as well as of its respective derivatives are listed in Table 1, Table 2 and Table 3. First of all, it can be noticed that all these molecules have pretty high values for dipole moments, compared to other aromatic molecules.4 This increase seems to be mainly due to the large electronegativity of the O atoms (resulting in large numerical values of the dipole moments of carbonyl groups) which amount to 4 Debye units in thiouracils, according to Schneider and Halverstadt 13 This value can be contributed to the relatively high polarity of the secondary amide carbonyl group in these compounds, as compared with the generally observed value of 2.23 Debye units.4 A pronounced change in the dipole moment is observed only upon the introduction of a substituent of a different polarity, such as Fluorine and Methyl group. In order to examine the effects of substituent on C5 on the electronic charge distribution in greater detail, many factors have to be taken into consideration. The first is that of electronegativity. Halogens are famously electronegative, with F atom being the most. The electronegativity of Fluorine atom pulls away electrons towards itself (and away from the ring) (Refer to Fig 3). As the dipole moment direction of ââ¬âF atom is directed towards itself, it somewhat cancels the dipole moment of N3. This explains why 5-Fluorouracil has a lower overall dipole moment compared to uracil. Thymine differs from uracil in having a methyl group (-CH3) on C5. The main chemistry to understand here is that of the inductive and mesomeric effect. ââ¬Å"Methylation at C5 and C6 mainly causes changes in the polarity of the C5C6 bond by way of increasing the ~-electronic charge on the atom at which substitution takes place.â⬠6 Due to the positive inductive effect of the ââ¬âCH3 group, electrons are pushed towards the aromatic ring. This adds to the ââ¬Ëelectron pullââ¬â¢ of N3 and contributes to the overall polarity of the molecule. It can be noted that substitution at C5 does not alter the dipole moment of uracil as much as a substituent on C6 would. (Since the substituents at C5 and C6 are differently oriented). For uracil, the dipole moment is directed in the N atom inbetween the carbonyl groups (as shown in Fig 3). However, the dipole moment is a more complicated calculation than can be inferred from a diagram as simple, lots of other data (such as bond angles) also have to be taken into account. Conclusion: The purpose of this experiment is to calculate the dipole moment of the anticancer drug, 5- fluorouracil, and compare its value with that of literature, and two other pyrimidines, thymine and uracil. Based on the data obtained with 5 FU, the experiment can be deemed to be successful, as it contains about 1-2 % error with respect to literature. In summary, we have demonstrated that these Gaussian calculations is an easy and convenient way to determine many physical and spectroscopic properties of these molecules in solution and can give an additional insight into their in vivo properties.1 Citations: Theoretical DFT and experimental NMR studies on uracil and 5- fluorouracil , B. Blicharska, T. Kupka / Journal of Molecular Structure 613 (2002) 153ââ¬â166 Frisch, M. J.et al. Gaussian Development Version, Revision D.02. In Gaussian Development Version, Revision D.02; Gaussian, Inc.: Wallingford CT, 2005 5-Fluorouracil and thymine form a crystalline solid solution, Sarah A. Barnett, Ashley T. Hulme* and Derek A. Tocher, Acta Crystallographica Section CVolume 62, Issue 7, Article first published online: 10 JUL 2006 L.A. Curtiss, M.S. Gordon Computational Material Chemistry: Methods and Applications, Kluwer Academic Publishers, 2004 Structures of the Molecular Components in DNA and RNA with Bond Lengths Interpreted as Sums of Atomic Covalent Radii Institute of Biophysics of the Academy of Sciences of the Czech Republic, Krà ¡lovopolskà ¡ 135, 61265 Brno, Czech Republic. Dipole moments of 2,4-diketopyrimidines: Part II: Uracil, thymine and their derivatives I. Kulakowskaa, M. Gellerb, B. Lesyngb, K.L. Wierzchowskia, Biochimica et Biophysica Acta (BBA) Nucleic Acids and Protein Synthesis Volume 361, Issue 2, 29 August 1974, Pages 119ââ¬â130 Chapter chemotherapy cancer http://www.oncoprof.net/Generale2000/g09_Chimiotherapie/Complements/g09_comp11.php (accessed Nov 19, 2014) Cole Parmer http://www.coleparmer.com/Product/5_Fluorouracil_99_5g/EW-88244-97 (accessed Nov 19, 2014) 5-Fluorouracil: mechanisms of action and clinical strategies, Daniel B. Longley1, D. Paul Harkin1 Patrick G. Johnston, Nature Reviews Cancer 3, 330-338 (May 2003) Wikipedia http://en.wikipedia.org/wiki/Fluorouracil (accessed 3rd December 2014) Hans-Dieter Hà ¶ltje, Gerd Folker, Molecular Modeling: Basic Principles and Applications, VCH Publishers, 1997 Vol. 5 Samakhvalov A, Lab Manual for Physical Chemistry I, Rutgers University Camden 2014 Schneider, W.C. and Halverstadt, I.F. (1948) J. Am. Chem. Soc. 70, 262626 1
Subscribe to:
Post Comments (Atom)
No comments:
Post a Comment
Note: Only a member of this blog may post a comment.