SlideShare una empresa de Scribd logo

NMR

Descargar como PPTX, PDF
Saurabh Negi
Saurabh Negi

NMR

Ciencias
1 de 18
NMR SPECTROSCOPY Prepared by: Saurabh Singh B. Pharma 4th year H.I.P.R Dehradun
THEORY Nuclear magnetic resonance (NMR) spectroscopy is the study of molecules by recording the interaction of radiofrequency (Rf), electromagnetic radiations with the nuclei of molecules placed in a strong magnetic field. “Zeeman first observed this type of activity in the end of 19th century, but practical use of the so called ZEEMAN EFFECT was only made in 1950s when NMR spectrometers are commercially available.
PRINCIPLE OF NMR SPECTROSCOPY • All nuclei are electrically charged and many have spin. • Transfer of energy is possible from base energy to higher energy levels when an external magnetic field is applied. • The transfer of energy occurs at a wavelength that coincides with the radio frequency. • Also, energy is emitted at the same frequency when the spin comes back to its base level. • Therefore, by measuring the signal which matches this transfer the processing of the NMR spectrum for the concerned nucleus is yield.
This instrument consists of nine major parts: 1. Sample holder – It is a glass tube which is 8.5 cm long and 0.3 cm in diameter. 2. Magnetic coils – Magnetic coil generates magnetic field whenever current flows through it 3. Permanent magnet – It helps in providing a homogenous magnetic field at 60 – 100 MHZ 4. Sweep generator – Modifies the strength of the magnetic field which is already applied. 5. Radiofrequency transmitter – It produces a powerful but short pulse of the radio waves. INSTRUMENTATION
WORKING OF NMR • Place the sample in a magnetic field. • Excite the nuclei sample into nuclear magnetic resonance with the help of waves to produce NMR signals. • These NMR signals are detected with sensitive radio receivers. • The resonance frequency of an atom in a molecule is changed by the intramolecular magnetic field surrounding it. • This gives details of a molecule’s individual functional groups and its electronic structure. • Nuclear magnetic resonance spectroscopy is a conclusive method of monomolecular organic compounds. • This method provides details of the reaction state, structure, chemical environment and dynamics of a molecule.
CHEMICAL SHIFT The chemical shift tells us about the magnetic field that the nucleus feels. The chemical shift in absolute terms is defined by the frequency of the resonance expressed with reference to a standard compound which is defined to be at 0 ppm. The scale is made more manageable by expressing it in parts per million (ppm) and is independent of the spectrometer frequency. It is often convenient to describe the relative positions of the resonances in an NMR spectrum. For example, a peak at a chemical shift, δ, of 10 ppm is said to be downfield or deshielded with respect to a peak at 5 ppm, or the peak at 5 ppm is upfield or shielded with respect to the peak at 10 ppm.
Factors affecting Chemical Shift Electronegativit y & Inductive Effect Hydrogen Bonding Vander Waals deshielding Anisotropic effect(Space Effect)
ELECTRONEGATIVITY & INDUCTIVE EFFECT • Greater the electronegativity, Greater is the deshielding • Delta value will be more HYDROGEN BONDING • Downfield shift depends upon the strength of H-bonding • Intra molecular H-bonding doesn’t show any shifting absorption VANDER WAALS DESHIELDING • Electron crowd of a bulky group will tend to repel the electron cloud (in over crowded molecules) surrounding the proton, & the proton is deshielded
ANISOTROPIC (SPACE) EFFECT • In a compound containing = or ≡ bond circulation of pi electrons about nearby nuclei generate an induced field which can either oppose or reinforce the location of proton or the space occupied by the proton. • The occurrence of shielding or deshielding can be determined by the location of proton in the space, that's why this effect is known as space effect. • Anisotropy is non-uniformity. • For different compounds this anisotropy is different as different distribution of electrons around nuclei. ALKENES • H+ deshielded. • Induced magnetic fluctuation (MF) – diamagnetic- act paramagnetic in the region of alkene proton. • H+ feels greater field strength. ALKYNES • H+ shielded. • Induced field opposes the applied field. • H+ feels smaller field strength.
3.SHIELDING AND DESHIELDING The basic principle of NMR is to apply an external magnetic field called B0 and measure the frequency at which the nucleus achieves resonance. Electrons orbiting around the nucleus generate a small magnetic field that opposes B0. In this case we say that electrons are shielding the nucleus from B0. Shielding: The higher the electron density around the nucleus, the higher the opposing magnetic field to B0 from the electrons, the greater the shielding. Because the proton experiences lower external magnetic field, it needs a lower frequency to achieve resonance, and therefore, the chemical shift shifts upfield (lower ppms) .
Deshielding: If the electron density around a nucleus decreases, the opposing magnetic field becomes small and therefore, the nucleus feels more the external magnetic field B0, and therefore it said to be deshielded. Because the proton experiences higher external magnetic field, it needs a higher frequency to achieve resonance, and therefore, the chemical shift shifts downfield (higher ppms) .
Comparison of the chemical shift of CH4 protons and CH3Cl protons: Chlorine atom is an electronegative atom that will pull the electron density toward it(electron withdrawing), resulting in a deshielding of the hydrogen nucleus; So it will fell higher external magnetic field B0 increasing the resonance frequency and therefore, shifting to higher ppms. Hydrogen nucleus is shielded in the case of CH4 and therefore, the peak appears on the lower ppm side.
SOLVENTS USED IN NMR CHARACTERSITICS OF SOLVENTS • Chemically inert • Solvents should be magnetically isotropic in nature • Free from any hydrogen(1 1H) atom • Solvent should be able to dissolve the molecule/sample in a reasonable quantity(approx. or more)  For dissolving polar compound – Polar solvent is used  For dissolving non-polar compound – Non-polar solvent is used. Commonly used solvents are:- The following solvents are normally used in which hydrogen may be replaced by deuterium. 1. Carbon tetrachloride – CCl4 2. Carbon disulphide – CS2 3. Deuterochloroform – CDCl3 4. Hexachloroacetone – {(CCl3)2CO} 5. Deuterobenzene – C6D6 6. Deuterium oxide – D2O
NMR SIGNAL FOR THE GIVEN COMPOUNDS a) C8H18 – Octane CH3 – (CH2)6 – CH3 NOW IT HAS ONLY ONE SIGNAL (B) (A) (B) Octane has two signals. b) C2H6O – Ethanol NOW IT HAS ONLY ONE SIGNAL Ethanol has 3 signals c) C5H12 – Pentane CH3 – (CH2)3 – CH3 NOW IT HAS ONLY ONE SIGNAL (B) (A) (B) Pentane has two signals. d) C4H12Si – Tetramethylsilane It has One signal. C C H 3 C H 3 C H 3 C C H 3 C H 3 C H 3 2 , 2 , 3 , 3 - t e t r a m e t h y l b u t a n e O C H 3 H 3 C m e t h o x y m e t h a n e C C H 3 C H 3 C H 3 H 3 C 2 , 2 - d i m e t h y l p r o p a n e S i C H 3 C H 3 C H 3 H 3 C t e t r a m e t h y l s i l a n e O H
REASON FOR DIFFERENT FREQUENCY OF PROTON MAGNETIC RESONANCE SIGNALS Since electrons are charged particles, they move in response to the external magnetic field (Bo) so as generate a secondary field that opposes the much stronger applied field. This secondary field shields the nucleus from the applied field, so Bo must be increased in order to achieve resonance (absorption of rf energy). Bo must be increased to compensate for the induced shielding field. The resonance condition ΔE = hν is satisfied when ΔE =fγB where B is the value of the magnetic field the H nucleus being observed. B can be regarded as having three components: 1. B0 the external applied magnetic field; 2. B1 the field due to electrons circulating near the nucleus being observed (i.e., chemical shift δ); 3. B2 the local magnetic field due to other magnetic nuclei (e.g. other H nuclei) near the observed H nucleus (i.e., J or spin-spin coupling).  So in general differently situated H nuclei resonate at different ν values. *(Note:- v = nu)
SPIN-SPIN COUPLING PATTERN FOR THE GIVEN MOLECULES ARE :- 1.CH3CHCl2 - There are two different chemical shifts for the H nuclei in this compound. The n+1 rule tells that for the CH3 group the single H nucleus in the adjacent CHCl2 group will split its signal into a 1:1 doublet (2 equal peaks). For the CHCl2 group the 3 protons in the adjacent CH3 group will split its signal into a quartet: four peaks of relative intensities 1:3:3:1. The total intensities of the two signals will be in the ratio 3:1. 2.CH3CHClCH3 - For the CHCl group the 6 equivalent H nuclei in the two adjacent and equivalent CH3 groups will give rise to a 7 peak signal ( a septet). For the two equivalent CH3 groups the single H nucleus in the CHCl group will give rise to an equal doublet signal. The total intensities of the two signals will be in the ratio of 1:6. 3.CH3OCH2CH3 - The ether oxygen with its bonds means that the magnetic effects of the sets of H nuclei on the two sides of the ether O are not transmitted through it. Thus the 3 H nuclei in the CH3O group give rise to one unsplit signal. For the OCH2CH3 group we expect a 1:3:3:1 quartet for the CH2 group and a 1:2:1 triplet for the CH3 group.
DIFFERENT CHEMICAL SHIFTS FOR THE GIVEN MOLECULES ARE :- 1. CH4 All H nuclei are equivalent since the molecule has a regular tetrahedral shape. Equivalent protons have the same chemical shift and do not give rise to J splitting. Only one chemical shift is expected. 2. CH3CH3 The chemical arrangement of molecule is the same as for CH4 and only one shift is expected. 3. CH3CH2CH3 The two terminal CH3 groups are magnetically and chemically equivalent and their hydrogen atoms will all have the same chemical shift. The central CH2 group is different and will give a resonance signal at a different chemical So two different chemical shifts are expected. 4. H2C=CH2 All H nuclei in this planar molecule are equivalent. Only one chemical shift is expected. 5. H2C=CHBr Each H nucleus in this planar molecule is different, it has three different molecules. So three chemical shifts are expected.
APPLICATION OF NMR SPECTROSCOPY • SOLUTION STRUCTURE • MOLECULAR DYNAMICS • PROTEIN FOLDING • IONIZATION STATE • PROTEIN HYDRATION • HYDROGEN BONDING • DRUG SCREENING AND DESIGN – Particularly useful for identifying drug leads and determining the conformations of the compounds bound to enzymes, receptors, and other proteins. • METABOLITE ANALYSIS – A very powerful technology for metabolite analysis. • CHEMICAL ANALYSIS – A matured technique for chemical identification and conformational analysis of chemicals whether synthetic or natural.

Recomendados

NMR, principle and instrumentation by kk sahu sir
NMR, principle and instrumentation by kk sahu sirNMR, principle and instrumentation by kk sahu sir
NMR, principle and instrumentation by kk sahu sir
KAUSHAL SAHU
 
Nuclear magnetic resonance (NMR)
Nuclear magnetic resonance (NMR)Nuclear magnetic resonance (NMR)
Nuclear magnetic resonance (NMR)
Maham Adnan
 
Nmr nuclear magnetic resonance spectroscopy
Nmr nuclear magnetic resonance spectroscopyNmr nuclear magnetic resonance spectroscopy
Nmr nuclear magnetic resonance spectroscopy
Joel Cornelio
 
NMR (Nuclear Magnetic Resonance)
NMR (Nuclear Magnetic Resonance)NMR (Nuclear Magnetic Resonance)
NMR (Nuclear Magnetic Resonance)
Shaheda Prvn
 
Nuclear magnetic resonance proton nmr
Nuclear magnetic resonance proton nmrNuclear magnetic resonance proton nmr
Nuclear magnetic resonance proton nmr
Sujit Patel
 
Factors affecting chemical shift
Factors affecting chemical shiftFactors affecting chemical shift
Factors affecting chemical shift
Vrushali Tambe
 
NMR SPECTROSCOPY
NMR SPECTROSCOPYNMR SPECTROSCOPY
NMR SPECTROSCOPY
PV. Viji
 
Electron spectroscopy
Electron spectroscopyElectron spectroscopy
Electron spectroscopy
Dharmendrapresentation
 

Recomendados

NMR, principle and instrumentation by kk sahu sir
NMR, principle and instrumentation by kk sahu sirNMR, principle and instrumentation by kk sahu sir
NMR, principle and instrumentation by kk sahu sir
KAUSHAL SAHU
 
Nuclear magnetic resonance (NMR)
Nuclear magnetic resonance (NMR)Nuclear magnetic resonance (NMR)
Nuclear magnetic resonance (NMR)
Maham Adnan
 
Nmr nuclear magnetic resonance spectroscopy
Nmr nuclear magnetic resonance spectroscopyNmr nuclear magnetic resonance spectroscopy
Nmr nuclear magnetic resonance spectroscopy
Joel Cornelio
 
NMR (Nuclear Magnetic Resonance)
NMR (Nuclear Magnetic Resonance)NMR (Nuclear Magnetic Resonance)
NMR (Nuclear Magnetic Resonance)
Shaheda Prvn
 
Nuclear magnetic resonance proton nmr
Nuclear magnetic resonance proton nmrNuclear magnetic resonance proton nmr
Nuclear magnetic resonance proton nmr
Sujit Patel
 
Factors affecting chemical shift
Factors affecting chemical shiftFactors affecting chemical shift
Factors affecting chemical shift
Vrushali Tambe
 
NMR SPECTROSCOPY
NMR SPECTROSCOPYNMR SPECTROSCOPY
NMR SPECTROSCOPY
PV. Viji
 
Electron spectroscopy
Electron spectroscopyElectron spectroscopy
Electron spectroscopy
Dharmendrapresentation
 
Raman spectroscopy
Raman spectroscopyRaman spectroscopy
Raman spectroscopy
suvarnayenduri
 
Introduction to NMR
Introduction to NMRIntroduction to NMR
Introduction to NMR
savvysahana
 
Raman spectroscopy
Raman spectroscopy Raman spectroscopy
Raman spectroscopy
Aravind AB
 
Raman spectroscopy
Raman spectroscopyRaman spectroscopy
Raman spectroscopy
Wilson Jefriyanto
 
FT NMR
FT NMRFT NMR
FT NMR
Rahul B S
 
X ray powder diffraction &
X ray powder diffraction &X ray powder diffraction &
X ray powder diffraction &
Arantha Jessy Joseph
 
Nuclear magnetic resonance final
Nuclear magnetic resonance finalNuclear magnetic resonance final
Nuclear magnetic resonance final
Aashish Patel
 
X ray diffraction
X ray diffractionX ray diffraction
X ray diffraction
Priyanka Jaiswal
 
Nuclear magnetic resonance (NMR) spectroscopy
Nuclear magnetic resonance (NMR) spectroscopyNuclear magnetic resonance (NMR) spectroscopy
Nuclear magnetic resonance (NMR) spectroscopy
VK VIKRAM VARMA
 
Raman spectroscopy
Raman spectroscopyRaman spectroscopy
Raman spectroscopy
Rawat DA Greatt
 
UV visible spectroscopy ( electronic spectroscopy)
UV visible spectroscopy ( electronic spectroscopy)UV visible spectroscopy ( electronic spectroscopy)
UV visible spectroscopy ( electronic spectroscopy)
ushaSanmugaraj
 
Nmr chemical shift, By Dr. UMESH KUMAR SHARMA AND ARATHY S A
Nmr chemical shift, By Dr. UMESH KUMAR SHARMA AND ARATHY S ANmr chemical shift, By Dr. UMESH KUMAR SHARMA AND ARATHY S A
Nmr chemical shift, By Dr. UMESH KUMAR SHARMA AND ARATHY S A
Dr. UMESH KUMAR SHARMA
 
Double resonance
Double resonanceDouble resonance
Double resonance
Priyanka Goswami
 
Raman spectroscopy by nitish kumar
Raman spectroscopy by nitish kumarRaman spectroscopy by nitish kumar
Raman spectroscopy by nitish kumar
NITISH KUMAR
 
Principle and working of Nmr spectroscopy
Principle and working of Nmr spectroscopyPrinciple and working of Nmr spectroscopy
Principle and working of Nmr spectroscopy
ArpitSuralkar
 
X ray diffraction ppt
X ray diffraction pptX ray diffraction ppt
X ray diffraction ppt
VanithaVaniN1
 
Raman spectroscopy (1)
Raman spectroscopy (1)Raman spectroscopy (1)
Raman spectroscopy (1)
MadhuraDatar
 
Nmr good
Nmr goodNmr good
Nmr good
Dr. Siju N Antony
 
x ray crystallography & diffraction
x ray crystallography & diffractionx ray crystallography & diffraction
x ray crystallography & diffraction
Arman Dalal
 
Nuclear magnetic Resonance(NMR) spectroscopy
Nuclear magnetic Resonance(NMR) spectroscopyNuclear magnetic Resonance(NMR) spectroscopy
Nuclear magnetic Resonance(NMR) spectroscopy
Preeti Choudhary
 
NMR
NMRNMR
NMR
SudhanshuMishra84
 
Nmr final
Nmr finalNmr final
Nmr final
SAURABHSHARMA1084
 

Más contenido relacionado

La actualidad más candente

Introduction to NMR
Introduction to NMRIntroduction to NMR
Introduction to NMR
savvysahana
 

La actualidad más candente (20)

Raman spectroscopy
Raman spectroscopyRaman spectroscopy
Raman spectroscopy
 
Introduction to NMR
Introduction to NMRIntroduction to NMR
Introduction to NMR
 
Raman spectroscopy
Raman spectroscopy Raman spectroscopy
Raman spectroscopy
 
Raman spectroscopy
Raman spectroscopyRaman spectroscopy
Raman spectroscopy
 
FT NMR
FT NMRFT NMR
FT NMR
 
X ray powder diffraction &
X ray powder diffraction &X ray powder diffraction &
X ray powder diffraction &
 
Nuclear magnetic resonance final
Nuclear magnetic resonance finalNuclear magnetic resonance final
Nuclear magnetic resonance final
 
X ray diffraction
X ray diffractionX ray diffraction
X ray diffraction
 
Nuclear magnetic resonance (NMR) spectroscopy
Nuclear magnetic resonance (NMR) spectroscopyNuclear magnetic resonance (NMR) spectroscopy
Nuclear magnetic resonance (NMR) spectroscopy
 
Raman spectroscopy
Raman spectroscopyRaman spectroscopy
Raman spectroscopy
 
UV visible spectroscopy ( electronic spectroscopy)
UV visible spectroscopy ( electronic spectroscopy)UV visible spectroscopy ( electronic spectroscopy)
UV visible spectroscopy ( electronic spectroscopy)
 
Nmr chemical shift, By Dr. UMESH KUMAR SHARMA AND ARATHY S A
Nmr chemical shift, By Dr. UMESH KUMAR SHARMA AND ARATHY S ANmr chemical shift, By Dr. UMESH KUMAR SHARMA AND ARATHY S A
Nmr chemical shift, By Dr. UMESH KUMAR SHARMA AND ARATHY S A
 
Double resonance
Double resonanceDouble resonance
Double resonance
 
Raman spectroscopy by nitish kumar
Raman spectroscopy by nitish kumarRaman spectroscopy by nitish kumar
Raman spectroscopy by nitish kumar
 
Principle and working of Nmr spectroscopy
Principle and working of Nmr spectroscopyPrinciple and working of Nmr spectroscopy
Principle and working of Nmr spectroscopy
 
X ray diffraction ppt
X ray diffraction pptX ray diffraction ppt
X ray diffraction ppt
 
Raman spectroscopy (1)
Raman spectroscopy (1)Raman spectroscopy (1)
Raman spectroscopy (1)
 
Nmr good
Nmr goodNmr good
Nmr good
 
x ray crystallography & diffraction
x ray crystallography & diffractionx ray crystallography & diffraction
x ray crystallography & diffraction
 
Nuclear magnetic Resonance(NMR) spectroscopy
Nuclear magnetic Resonance(NMR) spectroscopyNuclear magnetic Resonance(NMR) spectroscopy
Nuclear magnetic Resonance(NMR) spectroscopy
 

Similar a NMR

spectroscopy nmr for basic principles nmr
spectroscopy nmr for basic principles nmrspectroscopy nmr for basic principles nmr
spectroscopy nmr for basic principles nmr
prakashsaran1
 
NMR, principle, chemical shift , valu,13 C, application
NMR, principle, chemical shift , valu,13 C, applicationNMR, principle, chemical shift , valu,13 C, application
NMR, principle, chemical shift , valu,13 C, application
Tripura University
 
CHE-504 Lecture 3 Basics of NMR Spectroscopy by Dr. Charu C. Pant.pdf
CHE-504 Lecture 3 Basics of NMR Spectroscopy by Dr. Charu C. Pant.pdfCHE-504 Lecture 3 Basics of NMR Spectroscopy by Dr. Charu C. Pant.pdf
CHE-504 Lecture 3 Basics of NMR Spectroscopy by Dr. Charu C. Pant.pdf
TahreemFatima43565
 

Similar a NMR (20)

NMR
NMRNMR
NMR
 
Nmr final
Nmr finalNmr final
Nmr final
 
NMR spectroscopy
NMR spectroscopyNMR spectroscopy
NMR spectroscopy
 
spectroscopy nmr for basic principles nmr
spectroscopy nmr for basic principles nmrspectroscopy nmr for basic principles nmr
spectroscopy nmr for basic principles nmr
 
Nmr spectroscopy
Nmr spectroscopyNmr spectroscopy
Nmr spectroscopy
 
NMR, principle, chemical shift , valu,13 C, application
NMR, principle, chemical shift , valu,13 C, applicationNMR, principle, chemical shift , valu,13 C, application
NMR, principle, chemical shift , valu,13 C, application
 
NMR spectroscopy
NMR spectroscopy NMR spectroscopy
NMR spectroscopy
 
Nmr spectroscopy
Nmr spectroscopyNmr spectroscopy
Nmr spectroscopy
 
1H NMR Spectroscopy
1H NMR Spectroscopy1H NMR Spectroscopy
1H NMR Spectroscopy
 
NMR 7..pptx
NMR 7..pptxNMR 7..pptx
NMR 7..pptx
 
nmr spectroscopy and decription of nmr in details
nmr spectroscopy and decription of nmr in detailsnmr spectroscopy and decription of nmr in details
nmr spectroscopy and decription of nmr in details
 
Basics Principle of NMR
Basics Principle of NMRBasics Principle of NMR
Basics Principle of NMR
 
NMR
NMRNMR
NMR
 
CHE-504 Lecture 3 Basics of NMR Spectroscopy by Dr. Charu C. Pant.pdf
CHE-504 Lecture 3 Basics of NMR Spectroscopy by Dr. Charu C. Pant.pdfCHE-504 Lecture 3 Basics of NMR Spectroscopy by Dr. Charu C. Pant.pdf
CHE-504 Lecture 3 Basics of NMR Spectroscopy by Dr. Charu C. Pant.pdf
 
1H NUCLEAR MAGNETIC RESONANCE
1H NUCLEAR MAGNETIC RESONANCE1H NUCLEAR MAGNETIC RESONANCE
1H NUCLEAR MAGNETIC RESONANCE
 
Nuclear magnetic resonance by ayush kumawat
Nuclear magnetic resonance by ayush kumawatNuclear magnetic resonance by ayush kumawat
Nuclear magnetic resonance by ayush kumawat
 
Nmr2 pl
Nmr2 plNmr2 pl
Nmr2 pl
 
Nmr2 pl
Nmr2 plNmr2 pl
Nmr2 pl
 
Nmr lect
Nmr lectNmr lect
Nmr lect
 
Nmr lect
Nmr lectNmr lect
Nmr lect
 

Último

Asymmetry in the atmosphere of the ultra-hot Jupiter WASP-76 b
Asymmetry in the atmosphere of the ultra-hot Jupiter WASP-76 bAsymmetry in the atmosphere of the ultra-hot Jupiter WASP-76 b
Asymmetry in the atmosphere of the ultra-hot Jupiter WASP-76 b
Sérgio Sacani
 
THE ROLE OF BIOTECHNOLOGY IN THE ECONOMIC UPLIFT.pptx
THE ROLE OF BIOTECHNOLOGY IN THE ECONOMIC UPLIFT.pptxTHE ROLE OF BIOTECHNOLOGY IN THE ECONOMIC UPLIFT.pptx
THE ROLE OF BIOTECHNOLOGY IN THE ECONOMIC UPLIFT.pptx
ANSARKHAN96
 
CYTOGENETIC MAP................ ppt.pptx
CYTOGENETIC MAP................ ppt.pptxCYTOGENETIC MAP................ ppt.pptx
CYTOGENETIC MAP................ ppt.pptx
Silpa
 
Human genetics..........................pptx
Human genetics..........................pptxHuman genetics..........................pptx
Human genetics..........................pptx
Silpa
 
Cyathodium bryophyte: morphology, anatomy, reproduction etc.
Cyathodium bryophyte: morphology, anatomy, reproduction etc.Cyathodium bryophyte: morphology, anatomy, reproduction etc.
Cyathodium bryophyte: morphology, anatomy, reproduction etc.
Silpa
 
Phenolics: types, biosynthesis and functions.
Phenolics: types, biosynthesis and functions.Phenolics: types, biosynthesis and functions.
Phenolics: types, biosynthesis and functions.
Silpa
 
POGONATUM : morphology, anatomy, reproduction etc.
POGONATUM : morphology, anatomy, reproduction etc.POGONATUM : morphology, anatomy, reproduction etc.
POGONATUM : morphology, anatomy, reproduction etc.
Silpa
 

Último (20)

Cyanide resistant respiration pathway.pptx
Cyanide resistant respiration pathway.pptxCyanide resistant respiration pathway.pptx
Cyanide resistant respiration pathway.pptx
 
Asymmetry in the atmosphere of the ultra-hot Jupiter WASP-76 b
Asymmetry in the atmosphere of the ultra-hot Jupiter WASP-76 bAsymmetry in the atmosphere of the ultra-hot Jupiter WASP-76 b
Asymmetry in the atmosphere of the ultra-hot Jupiter WASP-76 b
 
Thyroid Physiology_Dr.E. Muralinath_ Associate Professor
Thyroid Physiology_Dr.E. Muralinath_ Associate ProfessorThyroid Physiology_Dr.E. Muralinath_ Associate Professor
Thyroid Physiology_Dr.E. Muralinath_ Associate Professor
 
PATNA CALL GIRLS 8617370543 LOW PRICE ESCORT SERVICE
PATNA CALL GIRLS 8617370543 LOW PRICE ESCORT SERVICEPATNA CALL GIRLS 8617370543 LOW PRICE ESCORT SERVICE
PATNA CALL GIRLS 8617370543 LOW PRICE ESCORT SERVICE
 
THE ROLE OF BIOTECHNOLOGY IN THE ECONOMIC UPLIFT.pptx
THE ROLE OF BIOTECHNOLOGY IN THE ECONOMIC UPLIFT.pptxTHE ROLE OF BIOTECHNOLOGY IN THE ECONOMIC UPLIFT.pptx
THE ROLE OF BIOTECHNOLOGY IN THE ECONOMIC UPLIFT.pptx
 
Human & Veterinary Respiratory Physilogy_DR.E.Muralinath_Associate Professor....
Human & Veterinary Respiratory Physilogy_DR.E.Muralinath_Associate Professor....Human & Veterinary Respiratory Physilogy_DR.E.Muralinath_Associate Professor....
Human & Veterinary Respiratory Physilogy_DR.E.Muralinath_Associate Professor....
 
module for grade 9 for distance learning
module for grade 9 for distance learningmodule for grade 9 for distance learning
module for grade 9 for distance learning
 
CYTOGENETIC MAP................ ppt.pptx
CYTOGENETIC MAP................ ppt.pptxCYTOGENETIC MAP................ ppt.pptx
CYTOGENETIC MAP................ ppt.pptx
 
FAIRSpectra - Enabling the FAIRification of Analytical Science
FAIRSpectra - Enabling the FAIRification of Analytical ScienceFAIRSpectra - Enabling the FAIRification of Analytical Science
FAIRSpectra - Enabling the FAIRification of Analytical Science
 
Human genetics..........................pptx
Human genetics..........................pptxHuman genetics..........................pptx
Human genetics..........................pptx
 
Genome sequencing,shotgun sequencing.pptx
Genome sequencing,shotgun sequencing.pptxGenome sequencing,shotgun sequencing.pptx
Genome sequencing,shotgun sequencing.pptx
 
Role of AI in seed science Predictive modelling and Beyond.pptx
Role of AI in seed science Predictive modelling and Beyond.pptxRole of AI in seed science Predictive modelling and Beyond.pptx
Role of AI in seed science Predictive modelling and Beyond.pptx
 
Site Acceptance Test .
Site Acceptance Test .Site Acceptance Test .
Site Acceptance Test .
 
Cyathodium bryophyte: morphology, anatomy, reproduction etc.
Cyathodium bryophyte: morphology, anatomy, reproduction etc.Cyathodium bryophyte: morphology, anatomy, reproduction etc.
Cyathodium bryophyte: morphology, anatomy, reproduction etc.
 
Use of mutants in understanding seedling development.pptx
Use of mutants in understanding seedling development.pptxUse of mutants in understanding seedling development.pptx
Use of mutants in understanding seedling development.pptx
 
Phenolics: types, biosynthesis and functions.
Phenolics: types, biosynthesis and functions.Phenolics: types, biosynthesis and functions.
Phenolics: types, biosynthesis and functions.
 
Proteomics: types, protein profiling steps etc.
Proteomics: types, protein profiling steps etc.Proteomics: types, protein profiling steps etc.
Proteomics: types, protein profiling steps etc.
 
Chemistry 5th semester paper 1st Notes.pdf
Chemistry 5th semester paper 1st Notes.pdfChemistry 5th semester paper 1st Notes.pdf
Chemistry 5th semester paper 1st Notes.pdf
 
POGONATUM : morphology, anatomy, reproduction etc.
POGONATUM : morphology, anatomy, reproduction etc.POGONATUM : morphology, anatomy, reproduction etc.
POGONATUM : morphology, anatomy, reproduction etc.
 
Atp synthase , Atp synthase complex 1 to 4.
Atp synthase , Atp synthase complex 1 to 4.Atp synthase , Atp synthase complex 1 to 4.
Atp synthase , Atp synthase complex 1 to 4.
 

NMR

  • 1. NMR SPECTROSCOPY Prepared by: Saurabh Singh B. Pharma 4th year H.I.P.R Dehradun
  • 2. THEORY Nuclear magnetic resonance (NMR) spectroscopy is the study of molecules by recording the interaction of radiofrequency (Rf), electromagnetic radiations with the nuclei of molecules placed in a strong magnetic field. “Zeeman first observed this type of activity in the end of 19th century, but practical use of the so called ZEEMAN EFFECT was only made in 1950s when NMR spectrometers are commercially available.
  • 3. PRINCIPLE OF NMR SPECTROSCOPY • All nuclei are electrically charged and many have spin. • Transfer of energy is possible from base energy to higher energy levels when an external magnetic field is applied. • The transfer of energy occurs at a wavelength that coincides with the radio frequency. • Also, energy is emitted at the same frequency when the spin comes back to its base level. • Therefore, by measuring the signal which matches this transfer the processing of the NMR spectrum for the concerned nucleus is yield.
  • 4. This instrument consists of nine major parts: 1. Sample holder – It is a glass tube which is 8.5 cm long and 0.3 cm in diameter. 2. Magnetic coils – Magnetic coil generates magnetic field whenever current flows through it 3. Permanent magnet – It helps in providing a homogenous magnetic field at 60 – 100 MHZ 4. Sweep generator – Modifies the strength of the magnetic field which is already applied. 5. Radiofrequency transmitter – It produces a powerful but short pulse of the radio waves. INSTRUMENTATION
  • 5. WORKING OF NMR • Place the sample in a magnetic field. • Excite the nuclei sample into nuclear magnetic resonance with the help of waves to produce NMR signals. • These NMR signals are detected with sensitive radio receivers. • The resonance frequency of an atom in a molecule is changed by the intramolecular magnetic field surrounding it. • This gives details of a molecule’s individual functional groups and its electronic structure. • Nuclear magnetic resonance spectroscopy is a conclusive method of monomolecular organic compounds. • This method provides details of the reaction state, structure, chemical environment and dynamics of a molecule.
  • 6. CHEMICAL SHIFT The chemical shift tells us about the magnetic field that the nucleus feels. The chemical shift in absolute terms is defined by the frequency of the resonance expressed with reference to a standard compound which is defined to be at 0 ppm. The scale is made more manageable by expressing it in parts per million (ppm) and is independent of the spectrometer frequency. It is often convenient to describe the relative positions of the resonances in an NMR spectrum. For example, a peak at a chemical shift, δ, of 10 ppm is said to be downfield or deshielded with respect to a peak at 5 ppm, or the peak at 5 ppm is upfield or shielded with respect to the peak at 10 ppm.
  • 7. Factors affecting Chemical Shift Electronegativit y & Inductive Effect Hydrogen Bonding Vander Waals deshielding Anisotropic effect(Space Effect)
  • 8. ELECTRONEGATIVITY & INDUCTIVE EFFECT • Greater the electronegativity, Greater is the deshielding • Delta value will be more HYDROGEN BONDING • Downfield shift depends upon the strength of H-bonding • Intra molecular H-bonding doesn’t show any shifting absorption VANDER WAALS DESHIELDING • Electron crowd of a bulky group will tend to repel the electron cloud (in over crowded molecules) surrounding the proton, & the proton is deshielded
  • 9. ANISOTROPIC (SPACE) EFFECT • In a compound containing = or ≡ bond circulation of pi electrons about nearby nuclei generate an induced field which can either oppose or reinforce the location of proton or the space occupied by the proton. • The occurrence of shielding or deshielding can be determined by the location of proton in the space, that's why this effect is known as space effect. • Anisotropy is non-uniformity. • For different compounds this anisotropy is different as different distribution of electrons around nuclei. ALKENES • H+ deshielded. • Induced magnetic fluctuation (MF) – diamagnetic- act paramagnetic in the region of alkene proton. • H+ feels greater field strength. ALKYNES • H+ shielded. • Induced field opposes the applied field. • H+ feels smaller field strength.
  • 10. 3.SHIELDING AND DESHIELDING The basic principle of NMR is to apply an external magnetic field called B0 and measure the frequency at which the nucleus achieves resonance. Electrons orbiting around the nucleus generate a small magnetic field that opposes B0. In this case we say that electrons are shielding the nucleus from B0. Shielding: The higher the electron density around the nucleus, the higher the opposing magnetic field to B0 from the electrons, the greater the shielding. Because the proton experiences lower external magnetic field, it needs a lower frequency to achieve resonance, and therefore, the chemical shift shifts upfield (lower ppms) .
  • 11. Deshielding: If the electron density around a nucleus decreases, the opposing magnetic field becomes small and therefore, the nucleus feels more the external magnetic field B0, and therefore it said to be deshielded. Because the proton experiences higher external magnetic field, it needs a higher frequency to achieve resonance, and therefore, the chemical shift shifts downfield (higher ppms) .
  • 12. Comparison of the chemical shift of CH4 protons and CH3Cl protons: Chlorine atom is an electronegative atom that will pull the electron density toward it(electron withdrawing), resulting in a deshielding of the hydrogen nucleus; So it will fell higher external magnetic field B0 increasing the resonance frequency and therefore, shifting to higher ppms. Hydrogen nucleus is shielded in the case of CH4 and therefore, the peak appears on the lower ppm side.
  • 13. SOLVENTS USED IN NMR CHARACTERSITICS OF SOLVENTS • Chemically inert • Solvents should be magnetically isotropic in nature • Free from any hydrogen(1 1H) atom • Solvent should be able to dissolve the molecule/sample in a reasonable quantity(approx. or more)  For dissolving polar compound – Polar solvent is used  For dissolving non-polar compound – Non-polar solvent is used. Commonly used solvents are:- The following solvents are normally used in which hydrogen may be replaced by deuterium. 1. Carbon tetrachloride – CCl4 2. Carbon disulphide – CS2 3. Deuterochloroform – CDCl3 4. Hexachloroacetone – {(CCl3)2CO} 5. Deuterobenzene – C6D6 6. Deuterium oxide – D2O
  • 14. NMR SIGNAL FOR THE GIVEN COMPOUNDS a) C8H18 – Octane CH3 – (CH2)6 – CH3 NOW IT HAS ONLY ONE SIGNAL (B) (A) (B) Octane has two signals. b) C2H6O – Ethanol NOW IT HAS ONLY ONE SIGNAL Ethanol has 3 signals c) C5H12 – Pentane CH3 – (CH2)3 – CH3 NOW IT HAS ONLY ONE SIGNAL (B) (A) (B) Pentane has two signals. d) C4H12Si – Tetramethylsilane It has One signal. C C H 3 C H 3 C H 3 C C H 3 C H 3 C H 3 2 , 2 , 3 , 3 - t e t r a m e t h y l b u t a n e O C H 3 H 3 C m e t h o x y m e t h a n e C C H 3 C H 3 C H 3 H 3 C 2 , 2 - d i m e t h y l p r o p a n e S i C H 3 C H 3 C H 3 H 3 C t e t r a m e t h y l s i l a n e O H
  • 15. REASON FOR DIFFERENT FREQUENCY OF PROTON MAGNETIC RESONANCE SIGNALS Since electrons are charged particles, they move in response to the external magnetic field (Bo) so as generate a secondary field that opposes the much stronger applied field. This secondary field shields the nucleus from the applied field, so Bo must be increased in order to achieve resonance (absorption of rf energy). Bo must be increased to compensate for the induced shielding field. The resonance condition ΔE = hν is satisfied when ΔE =fγB where B is the value of the magnetic field the H nucleus being observed. B can be regarded as having three components: 1. B0 the external applied magnetic field; 2. B1 the field due to electrons circulating near the nucleus being observed (i.e., chemical shift δ); 3. B2 the local magnetic field due to other magnetic nuclei (e.g. other H nuclei) near the observed H nucleus (i.e., J or spin-spin coupling).  So in general differently situated H nuclei resonate at different ν values. *(Note:- v = nu)
  • 16. SPIN-SPIN COUPLING PATTERN FOR THE GIVEN MOLECULES ARE :- 1.CH3CHCl2 - There are two different chemical shifts for the H nuclei in this compound. The n+1 rule tells that for the CH3 group the single H nucleus in the adjacent CHCl2 group will split its signal into a 1:1 doublet (2 equal peaks). For the CHCl2 group the 3 protons in the adjacent CH3 group will split its signal into a quartet: four peaks of relative intensities 1:3:3:1. The total intensities of the two signals will be in the ratio 3:1. 2.CH3CHClCH3 - For the CHCl group the 6 equivalent H nuclei in the two adjacent and equivalent CH3 groups will give rise to a 7 peak signal ( a septet). For the two equivalent CH3 groups the single H nucleus in the CHCl group will give rise to an equal doublet signal. The total intensities of the two signals will be in the ratio of 1:6. 3.CH3OCH2CH3 - The ether oxygen with its bonds means that the magnetic effects of the sets of H nuclei on the two sides of the ether O are not transmitted through it. Thus the 3 H nuclei in the CH3O group give rise to one unsplit signal. For the OCH2CH3 group we expect a 1:3:3:1 quartet for the CH2 group and a 1:2:1 triplet for the CH3 group.
  • 17. DIFFERENT CHEMICAL SHIFTS FOR THE GIVEN MOLECULES ARE :- 1. CH4 All H nuclei are equivalent since the molecule has a regular tetrahedral shape. Equivalent protons have the same chemical shift and do not give rise to J splitting. Only one chemical shift is expected. 2. CH3CH3 The chemical arrangement of molecule is the same as for CH4 and only one shift is expected. 3. CH3CH2CH3 The two terminal CH3 groups are magnetically and chemically equivalent and their hydrogen atoms will all have the same chemical shift. The central CH2 group is different and will give a resonance signal at a different chemical So two different chemical shifts are expected. 4. H2C=CH2 All H nuclei in this planar molecule are equivalent. Only one chemical shift is expected. 5. H2C=CHBr Each H nucleus in this planar molecule is different, it has three different molecules. So three chemical shifts are expected.
  • 18. APPLICATION OF NMR SPECTROSCOPY • SOLUTION STRUCTURE • MOLECULAR DYNAMICS • PROTEIN FOLDING • IONIZATION STATE • PROTEIN HYDRATION • HYDROGEN BONDING • DRUG SCREENING AND DESIGN – Particularly useful for identifying drug leads and determining the conformations of the compounds bound to enzymes, receptors, and other proteins. • METABOLITE ANALYSIS – A very powerful technology for metabolite analysis. • CHEMICAL ANALYSIS – A matured technique for chemical identification and conformational analysis of chemicals whether synthetic or natural.