AN ABSTRACT OF THE THESIS OF

YILIN QIAO for the Master of Science

in Chemistry presented on September 1st, 1994.

Title: Synthesis of substituted Planar Triarylmethane.

Abstract approved:

Two protective groups, benzyl and butyl, were utilized to

protect the central carbon of sesquixanthene in electrophilic

sUbstitution reactions. Attempts were also made to perform

sUbstitution on unprotected sesquixanthene.

Nitration was carried out on sesquixanthene where the

central carbon was protected and where the central carbon was

unprotected. After bromination and nitration, cleavage of the

protective group by oxidation was successful. Reduction of the

nitro groups to amino groups by tin metal and stannous

chloride was also attempted, but because of inavailability of

necessary analytical methods, the results were inconclusive.

_ ------1

SYNTHESIS OF SUBSTITUTED

PLANAR TRIARYLMETHANES

A Thesis

Presented to

the Department of Chemistry

EMPORIA STATE UNIVERSITY

In Partial Fulfillment

of the Requirements for the Degree

Master of Science

by

Yilin Qiao ~

September 1994

~ 1

,<

ACKNOWLEDGEMENT

I would like to express my deepest thanks to my thesis

advisor and committee chair, Dr. Eric Trump, for the guidance

of my research project and my graduate study. He was always

willing to answer any questions that I might have about the

SUbject matter of this thesis. without his encouragement, this

thesis would never have been completed.

I would also like to express my sincere gratitude to my

academic advisor, Dr. Charles Greenlief, for his suggestions

and for his devoting time and tolerance to give all kinds of

help.

I would like to voice my appreciations to Dr. Robert

Jones for devoting his valuable time to give advice and to

review my thesis.

I would like to express my sincere gratitude to Dr.

Arthur Landis and Dr. Kenneth Johnson for instructions in

using certain instrumentation.

"'"'-------­

i

CONTENTS

INTRODUCTION••••••••••••••••••••••••••••••••••••••••••••••••• 1

EXPERIMENTAL SECTION••••••••••••••••••••••••••••••••••••••••• 6

2,6,2',6',2.. ,6..-hexamethoxytriphenylcarbinol •••••••••••••• 6

9-(2,6-dimethoxyphenyl)-1,8-dimethoXYXanthydrol ••••••••••• 7

sesquixanthydrol 8

a. From 2,6,2',6',2.. ,6..-hexamethoxytriphenylcarbinol. •••• 8

b. From 9-(2,6-dimethoxyphenyl)-1,8-dimethoxyxanthydrol •• 8

Benzyl sesquixanthene and butyl sesquixanthene••••••••••• 10

a. Reaction with fluoroboric acid ••••••••••••••••••••••• 10

b. Reaction with benzyl magnesium chloride•••••••••••••• 10

c. Reaction with butyl magnesium bromide •••••••••••••••• 11

Benzyl tribromosesquixanthene•••••••••••••••••••••••••••• 12

Butyl tribromosesquixanthene••••••••••••••••••••••••••••• 12

cleavageofprotectinggroup•••••••••••••••••••• . •.• .. 13

Fluoroboric trinitrosesquixanthene••••••••••••••••••••••• 14

Reductionoffluoroborictrinitrosesquixanthene •• • .15

Butyl trinitrosesquixanthene•••••••••••••••••••• • .15

Reductionofbutyltrinitrosesquixanthene•••••••••• • •• 15

DISCUSSION OF RESULTS ••••••••••••••••••••••••••••••••••••••• 17

CONCLUSION•••••••••••••••••••••••••••••••••••••••••••••••••• 23

REFERENCES. • • • • • • • • • • • • • • • • • • • • • • • • • • • • • • • • • • • • • • • • • • • • • • • • • 2 4

IR SPECTRA••••••••• • .26

NMR. SPECTRA••••••••••••••••••••••••••••••••••••••••••••••••• 41

"'---­

ii

LIST OF IR SPECTRA

1. IR spectrum of 2,6,2',6',2",6"­hexamethoxytriphenylcarbinol ••••••••••••••••••••••••••. 26

2. IR spectrum of 9-(2,6-dimethoxyphenyl)­1,8-dimethoXYXanthydrol•••••••••••••••••••••••••••••••• 27

3. IRspectrumofsesquixanthydrol •••••••••••••••••••••••• 28

4. IR spectrum of fluroboric sesquixanthene ••••••••••••••• 29

5. IR spectrum of benzyl sesquixanthene ••••••••••••••••••• 30

6. IR spectrum of butyl sesquixanthene•••••••••••••••••••• 31

7. IR spectrum of the product obtained from bromination of benzyl sesquixanthene••••••••••••••••••••••••••••••• 32

8. IR spectrum of product obtained from bromination of butyl sesquixanthene•••••••••••••••••••••••••••••••• 33

9. IR spectrum of the product obtained from oxidation of benzyl trinitrosesquixanthene••••••••••••••••••••••. 34

10. IR spectrum of the product obtained from nitration of fluoroboric sesquixanthene•••••••••••••••••••••••••. 35

11. IR spectrum of the product obtained from reduction of fluoroboric trinitrosesquixanthene•••••••••••••••.•. 36

12. IR spectrum of the product obtained from nitration of butyl sesquixanthene•••••••••••••••••••••••••••••••• 37

13. IR spectrum of the product obtained from reduction reactionofbutyltribromosesquixanthene ••••••••••••••• 38

14. IR spectrum of the product obtained from nitration reactionofbenzylsesquixanthene •••••••••••••••••••••. 39

15. IR spectrum of the product obtained from bromination of fluoroboric sesquixanthene•••••••••••••••••••••••••. 40

1""'"""--­

iii

LIST OF NMR SPECTRA

16. NMR spectrum of the solvent deuterated chloroform•••••• 41

17. NMR spectrum of the solvent deuterated acetone ••••••••• 42

18. NMR spectrum of 9-(2,6-dimethoxyphenyl)­1,8-dimethoxyxanthydrol•••••••••••••••••••••••••••••••• 43

19. NMR spectrum of sesquixanthydrol ••••••••••••••••••••••• 44

20. NMR spectrum of benzyl sesquixanthene•••••••••••••••••• 45

21. NMR spectrum of butyl sesquixanthene••••••••••••••••••• 46

22. NMR spectrum of the product obtained from bromination of benzyl sesquixanthene••••••••••••••••••••••••••••••• 47

23. NMR spectrum of the product obtained from nitration of fluroboric sesquixanthene••••••••••••••••••••••••••• 48

........

----

1

INTRODUCTION

Triarylmethane dyes have been used in many areas of

chemistry. They are useful reagents for indicators, 1

dichromatic titration and redox indicators, determining the

presence of traces of halide irons,2 and the

spectrophotometric determination of Sb(III),3 Ta(V)," Ga(III),s

In,6 to list just a few. They are used in ball point pen inks'

and as corrosion inhibitors.' Several triarylmethane dyes are

good indicators of the titration for Fe(II), Ti(III), Cr(II),

Cu(I) with Ce(IV), and for the titration of Fe(II), Fe(CN):,

U(IV), Mo(V) and hydroquinone with dichromate.

Except for the azodyes, triphenylmethane and xanthene

dyes are the most commonly used reagents in the

spectrophotometric determination of metals. Reports on the

most common and well known sUbstances--aluminon,

phenylfluorone, malachite green, brilliant green, crystal

violet, and rhodamine--were published over a half century ago.

In the phenol red group, for example, phenolsulfonphthalein

has been used for the kinetic determination of copper,' the

decomposition of the dye being recorded

spectrophotometrically.

Two problems with these indicators are that their

reactions are not all reversible and they are often not stable

in oxidizing solutions. In spite of these disadvantages, they

have been commonly used. 10,11

2

The unique properties of the central carbon atom have

aroused much chemical interest in triarylmethane dyes. A free

radical, a cation, or an anion can occupy the central

position, with resonance delocalization on the aromatic rings.

The stabilization of triarylmethane dyes is dependent on the

degree of twist of three phenyl rings. The dye has maximum

stability when the rings are coplanar, but this is normally

impossible, so a propeller-shaped molecule results. 12,13

The stability of triarylmethanes is also dependent on the

ring substituents. Ortho-substitution decreases the

stabilization because of large steric effect. The cation of

this para-methyl substituted triarylmethane is five times as

stable as the cation of tris ortho-methyl substituted

triarylmethane. 14 It may be seen that the effect of ortho

substitution is large and the effect is most readily

attributed to steric factors. Increasing the degree of ring

twist will decrease the degree of ring resonance and thus

decrease stabilization.

The use of oxygen bridges to force planarity of

triarylmethane or triaryl radicals has been investigated and

numerous 9-substituted xanthyl (I) free radicals have been

reported by conant. IS stability increased because of the oxygen

bridges. The two oxygen bridged molecule (II) in the xanthyl

series has also been reported. 16 This radical was reported to

be 100% dissociated in benzene at room temperature since

dilute solutions of the radical were found to obey Beer's law

"'""----­

3

and no darkening of the solution occurred on warming. The

authors have interpreted this high degree of dissociation as

being due to high resonance stabilization in the free radical

due to planarity of the system. When compound (II) is compared

with compound (I), it is observed that compound (II) shows

greater stabilization due to second oxygen bridge.

o

(I) (II )

sesquixanthydrol (III) was of considerable synthetic and

chemical interest to us. It has an unusually high basicity

caused by resonance distribution of the positive charge to the

oxygen bridge as shown in structure (IV).

o o

o

(III )

0+

(IV)

""-----­

4

In a sUfficiently acidic solution, sesquixanthydryl is

protonated and loses water. This type of compound is called a

"secondary base" and the equilibrium constant is expressed in

terms of KR + .18 Triphenylcarbinol, has a pKR + of -6.63. 19 Based

on the differences between the resonance structure of

triarylmethane and sesquixanthene, the pKR+ for sesquixanthene

is expected to be much larger than -6.63. Generally, electron

donating groups should stabilize the carbonium ion and

increase pKR+. Three para dimethylamino groups increase the

pKR+ to 9.63 and three para methoxy groups change the pKR+ to

0.82.

The planar sesquixanthydryl cation (IV) is noted for its

exceptional stability. Propeller-shaped crystal violet (V),

which contains electron-donating dialkylamino groups, is noted

for its intense color, but it is not fluorescent. In

fluorescent Rhodamine B(VI),2° which contains dialkylamino

groups, two of the three rings are locked into the same plane

by an oxygen bridge. Combining the planarity of the

sesquixanthydryl cation with electron donating group such as

crystal violet (V) produces compound such as triamino­

sesquixanthene (VII) is the objective of our research. Such a

series of compounds would be expected to be intensely colored

and strongly fluorescent.

A known synthetic route21 for the preparation of amino

substituted sesquixanthene dyes is to start with a substituted

benzene which has a good leaving group, such as 3,5-dimethoxy

(CH 3 CH 2 ) 2 N o

:.J---C -OH

+ N(CH 2 CH3 )2

5

fluorobenzene. This route avoids protecting the central

carbonium ion. Our primary purpose was to create a different

synthetic route which would allow us to synthesize the

sesquixanthene base first and then add protecting group to

form a sesquixanthene dye as an intermediate, then to replace

a hydrogen on the aromatic ring with an amino group, forming

a basic amino dye. When this synthesis was carried out, we had

the opportunity to investigate the activity of the central

carbon, the protective ability of different substituted

groups, and the relationship between fluorescence and color.

~H3)2

~ o

a N(CH 3 )2(CH 3 )2 N .//

( V)

H N NH2 2 (VII) ~

o 1/

(VI)

"-­

6

EXPERIMENT SECTION

OCH3H3 CO

H3CDCH3 H3c6iCH3 + I Li) I

~ ~6 H3CO~OCH3

synthesis of 2,6,2',6',2",6"-hexamethoxytriphenylcarbinol

-

cx:::H3I -t CH30-~-OCH3 ~ ~

~./'1 ~

H3m cx:::H3

A solution of phenyl lithium was prepared by the addition

of bromobenzene (19.5 g,0.125 mole) to 65 mL of ether with

lithium wire (2.0 9 0.290 mole) and 30 mL of diethyl ether.

1,3-dimethyl benzene (15.0 g, 0.109 mole) was added and the

reaction mixture was allowed to stand at room temperature

under an atmosphere of nitrogen for sixty hours. 2, 6-dimethoxy

phenyl lithium was formed as white crystals. 29 Dimethyl

carbonate (3.24 g, 0.036 mole) in 200 mL of benzene was added

and the reaction mixture was refluxed for three days under a

protective nitrogen atmosphere. A white solid formed in the

reaction mixture during this time. After cooling, the reaction

mixture was poured into 300 mL of water to produce an aqueous

-

7

layer and an organic layer. The organic layer was separated

from the aqueous layer, washed twice with water, dried over

sodium sulfate and concentrated to yield a grey residue. The

residue was recrystallized once from ether to yield 14.98 g

(47%) of 2,6,2',6',2", 6"-hexamethoxytriphenyl carbinol with

melting point 163-164°C. The product was verified by IR

spectrum Figure 1.

Synthesis of 9-(2,6-dimethoxyphenyll-1,8-dimethoxyxanthydrol

OCH3

CH3~HCl

OCH3

CH3

A solution of 2,6,2',6',2",6"­

hexamethoxytriphenylcarbinol (4.0 g, 0.0508 mole) in 1,000 mL

of water and 10 mL of concentrated hydrochloric acid was

heated for two hours on a sand bath. The initial deep purple

solution became deep red during the reaction and a white

precipitate formed. The precipitate was collected by suction

filtration and dried under vacuum to yield 3.48 g (96%) of 9­

(2,6-dimethoxyphenyl)-1,8-dimethoxyxanthydrol. The product

was purified by one recrystallization from benzene-acetone to

give 2.58g of material with melting point 295-298°C. This

"

8

and

o

0.435 mole)(50.0 q,

Cl

oH-N+

H 3

CO OCH 3

~/i ~

pyridine hydrochloride

A. from 2,6,2',6',2 1 ,6"-hexamethoxytriphenylcarbinol

spectrum Figure 18.

2,6,2' ,6' ,2 1 ,6"-hexamethoxytriphenylcarbinol (10.0 q, 0.023

was identified by infrared spectrum Figure 2. and NMR

synthesis of sesquixanthydrol:

-­

mole) were mixed and heated with stirrinq at 195°C for one

hour. The initial purple mass qradually became liquid under

these conditions and took on a red color. The reaction mixture

was washed into one litter of water to produce a red solid and

a yellow aqueous solution. The solution was filtered to remove

the red solid and was then basified with potassium hydroxide

to produce a white solid. This product was purified by

recrystallization from a solution of diethyl ether, benzene,

and ethanol to yield 0.9 q of pure material which was

identified as sesquixanthydrol.

B. from 9-(2,6-dimethoxyphenyl)-1,8-dimethoxyxanthydrol

9

The product wassesquixanthydrol.of

CH 3 0 0' ~ '0

OCH 3

.;.:-..... I >

+N I

H U­

(89%)g

basified with potassium hydroxide Which discharged the yellow

were mixed and heated at maximum reflux on a sand bath for one

9-(2,6-dimethoxyphenyl)-1,8-dimethoxyxanthydrol (2.5 g,

0.006 mole) and pyridine hydrochloride (7.0 g, 0.061 mole)

hour. The initial solid became a deep red liquid. At the end

1.75

washed out with water. A red solid remained undissolved in the

water and the solids remaining in the reaction flask were

color of the solution and produced a light brown precipitate.

water while the solution was a reddish yellow color. The

aluminum absorption column to yield 1.17 g (65%) of white pure

of this time, the red liquid reaction product was poured into

solution was filtered to remove the red material and was then

The precipitate was collected and dried under vacuum to yield

recrystallized once from ether, purified by passing it through

.....

sesquixanthydrol with melting point 303°C. The product was

verified by Infrared spectrum Figure 3, and NMR spectrum

10

7+ HBF 4

b. Reaction with benzyl magnesium chloride.

(rH2Cl. ) OCH:>"9Cl

Mg

~

d9C' OCE

0

Sesquixanthydrol (2.0 g, 0.007 mole) was dissolved in 200

a. Reaction with fluoroboric acid.

synthesis of benzyl sesquixanthene and butyl sesquixanthene.

in the presence of acetic anhydride. The reaction mixture was

ml ether and fluoroboric acid (1.75 ml, 0.014 mole) was added

Figure 19.

point above 350°C. verified by infrared spectrum Figure 4.

stirred at room temperature for one hour. A yellow colored

solid gradually formed. The solution was separated by suction

filtration, and the solid was washed with 20 Xl benzene to

yield 2.3 g (94%) of fluoboric sesquixanthydrol with melting

...

Fluoboric sesquixanthene (0.8 g, 0.002 mole) was added in

70 mL of ethyl ether. Freshly prepared butyl magnesium bromide

was added dropwise under nitrogen with stirring. The yellow

CI-l 3

CH 2 CH 2 CH 3

o

o

CH 3

CH2

CH 2 CH 2 Br

CH 3

CH 2

CH 2

cH 2MgBr?

~

CH 3

CH 2

CH 2

cH 2

MgBr ~

+ Br

+ Mg

o

CIl 3

CH 2

CH 2

cH 2m:

CH 3

CH 2

CH 2

cH 2 Br

11

Fluroboric sesquixanthene (1.7 g, 0.0046 mole) was added

to 100 mL of diethyl ether. Freshly prepared benzyl magnesium

chloride was added dropwise under nitrogen while stirring. The

yellow solid disappeared gradually. The solution was allowed

to stand for 30 minutes after all solid had disappeared. The

solution was washed using 40% concentrated HCl. The organic

layer was separated from the aqueous layer, washed once with

water, dried over sodium sulfate and concentrated to yield a

light brown solid. The brown solid was recrystallized once

from hexane to yield 1.45 g (84%) of pure benzyl

sesquixanthydrol with melting point 173-175°C. The product was

analyzed spectroscopically using IR and NMR, giving the

infrared spectrum Figure 5, and NMR spectrum Figure 20.

c. Reaction with butyl magnesium bromide.

12

solid disappeared gradually. The solution was allowed to stand

for 30 minutes after all the solid disappeared. The solution

was washed with 10% hydrochloric acid. The organic layer was

separated from aqueous layer, washed once with water, dried

over sodium sUlfate and concentrated to yield a light brown

solid. The brown solid was recrystallized once from hexane to

yield 0.7 g (95%) of white, pure butyl sesquixanthene with

melting point 161-161. 5°C. The product was analyzed

spectroscopically using IR and NMR, giving the infrared

spectrum Figure 6 and NMR spectrum Figure 21.

synthesis of 1,1' ,1"-tribromo-benzyl sesquixanthene I 1,1' ,1"­

tribromo butyl sesquixanthene:

>CH 2 { > + Br2 ~

Br

CH 2 {

Br

Finely powdered benzyl sesquixanthene or butyl

sesquixanthene was placed in a weighing bottle cover, and then

the bottle cover was placed in a large neck Erlenmeyer flask

(the ideal vessel is a desiccator). Another weighing bottle

cover containing chemical quantitative bromine liquid (neat)

was set side by side with weighing bottle cover in the

,

13

butyl

o

Br

For tribromo benzyl

H+ KMno~

benzyl sesquixanthene I

Br

B;H -O~ 2_

o

In the flask,

A solution was prepared by adding 1,1' ,1"-tribromo benzyl

Erlenmeyer flask and its contents was allowed to stand 8 hours

Erlenmeyer flask. A rubber stopper sealed the erlenmeyer

Erlenmeyer flask and allowed to stand in the air under the

hydrogen bromide. The orange solid was then removed from the

or overnight. During this period, a needle was inserted, at

flask.

30 JIlL of benzene, filtered and cooled in an ice-bath. The

two hour intervals, to provide a means of escape for the

hood for four hours to allow the evaporation of bromine. The

crude 2,2',2"-tribromo benzyl sesquixanthene was dissolved in

products were light pink color.

sesquixanthene was in contact with bromine vapor. The

NMR spectrum Figure 22.

sesquixanthene, the melting point was 261°C and for butyl

tribromosesquixanthene, the melting point was 220°C. The

products were analyzed by IR spectrum, Figures 7 and 8, and

resulting crystals were filtered and air dried. Both of the

Cleavage of protective group.

14

sesquixanthene (0 .1S g, 0.0003 mole) in so mL of diethyl

ether, potassium permanganate (0.14 g, 0.0009 mole) in 20 mL

of water, and 2 mL of sulfuric acid. The mixture was allowed

to reflux overnight. At the end of the reaction, a white solid

product was formed between the ether and aqueous layers. The

solid mixture was collected by suction filtration and then

poured into ethyl ether with stirring for ten minutes. The

ether insoluble portion was separated by suction filtration.

The ether layer was dried over sodium sulfate and concentrated

to yield a white solid with melting point at 30SoC. This

product was analyzed by IR spectrum and this spectrum is shown

in Figure 9.

synthesis of Fluroboric trinitrosesquixanthene.

HNOJ ~

N02

Fluroboric sesquixanthene 0.6 g, 0.0016 mole) was placed

in an Erlenmeyer flask, and 30 mL of concentrated nitric acid

was added. The Erlenmeyer flask was heated and maintained in

a SO°C water bath for two hours. After cooling, a small

portion was dried in air. A needle-shaped product was formed.

The rest was poured into 100 mL of crushed ice. At this time,

"­

15

a golden orange colored solid was formed. The product was

collected by suction filtration, dried in 800e oven to yield

0.39 g, 0.0009 mole (59%) of the product, which was platelet

shaped with a melting point above 350oe. The product was

analyzed by IR in Figure 10 and NMR in Figure 23. A test by

iron (II) hydroxide was positive.

Reduction reaction of fluoroboric trinitrosesquixanthene.

The procedure of reducing the fluoroboric

trinitrosesquixanthene was the same as the procedure for the

reduction reaction of butyl trinitrosesquixanthene, but the

color of the product was different. The melting point was

above 360oe. The IR spectrum is presented in Figure 11.

synthesis of Butyl trinitrosesquixanthene.

The nitration procedure with butyl sesquixanthene was

almost the same as the procedure for the nitration reaction

of fluoroboric sesquixanthene. The only difference was that a

little sUlfuric acid was added. The melting point was 292­

296°e. The product was analyzed by IR spectrum, Figure 12.

Reduction of butyl trinitrosesquixanthene.

Butyl trini trosesquixanthene (1.32 gO. 003 mole) was

placed in round-bottomed flask which was fitted with a reflux

condenser. 100 mL of concentrated hydrochloric acid was added.

The mixture was heated with vigorous stirring in order to

dissolve the fluoroboric trinitrosesquixanthene. After the

solid dissolved (it was difficult to dissolve all of the

solid), granulated tin metal (2.5 g, 0.02 mole) was added in

16

very small portions during a 6 hours period. After adding tin

metal, the color of the solution changed from yellow to

orange. When the reaction was complete, an orange solid

precipitated. As the reaction mixture cooled, the product was

separated by suction filtration. The solid portion was washed

with 20 mL of water and dried in the air at 110°C to yield

(0.56 g, 50%) a reddish orange colored powder with a melting

point of 219-222°C. This product did not dissolve in ether, or

benzene, but was slightly soluble in water. The IR spectrum of

the product shown in Figure 13.

17

DISCUSSION

There are two possible precursors to sesquixanthydrol.

Both are alcohols, the structures are shown as (I) and (II).

H CO OCH 33

H CO OCH 33(II)( I )

Of these two precursors, (I) is much more viable, as (II) is

formed only with great difficulty.

In considering synthetic routes to sesquixanthydrol the

most promising method utilized a ring closure reaction. 22

pyridine hydrochloride appears to be the most effective ring

closure agent for this reaction. Since the alcohol (II)

eXhibits large steric hindrance due to the methoxy groups, the

conditions for ring closur. of compound (II) were extremely

difficult to optimize. The synthetic route from alcohol (II)

was abandoned at this point and attempts were directed toward

a synthesis of alcohol(I), for which steric factors are less

extreme.

2,2' , 6' ,2", 6"-dimethoxytriphenylcarbinol is very acid

sensitive. It formed appreciable amounts of the deep purple

:.

18

cation even in distilled water. In ethyl ether, its initial

colorless solution rapidly changed to purple while evaporating

the ether in the atmosphere. It is water soluble, but also

slightly soluble in ether and benzene. Not only is it a deep

purple color but also a high adhesive ability as well. At low

pH, it will lose two of its methoxy groups and form one oxygen

bridge.

It is important to protect the central carbonium ion in

ring substitution reactions. since the central carboxyl group

is extremely active and easy to oxidize, it must be protected

by a group such as benzyl or n-butyl. Two Grignard reagents,

benzyl magnesium chloride and butyl magnesium bromide, were

successfully made and successfully reacted with sesquixanthyl

fluoroborate forming benzyl sesquixanthene and butyl

sesquixanthene. The protection of the central carbon seemed

perfect.

Two routes were designed to synthesize tris-4,4'4"-amino

sesquixanthene. One involved the synthesis of tris-4, 4' 4"­

nitro sesquixanthene intermediate, and then, the subsequent

reduction of the nitro groups to amino groups. The other

involved halogenation of the phenyl rings first, then utilized

the benzyne mechanism to replace the halogens by amino groups.

The halogenation followed by benzyne elimination-addition was

expected to give a higher yield of the desired product,

4,4',4"-triamino sesquixanthene.

Nitration or halogenation were expected to be easy to

'--~

19

carry out. Theoretically, the ether groups should be strongly

activating. On the other hand, when the central carbon carries

a positive change, the rings should be deactivated with

respect to electrophilic sUbstitution.

Bromination of benzyl sesquixanthene in ethyl ether was

unsuccessful. When benzyl sesquixanthene was allowed to stand

with bromine for three days, the reactants retained their

yellow color and looked the same as the starting material even

in the presence of ferric chloride. We believe that 1,1',1"­

bromo benzyl sesquixanthene should be white.

Bromination of benzyl sesquixanthene and butyl

sesquixanthene by bromine vapor was successful. The product of

the bromination reaction was analyzed by IR. From the IR

spectrum, Figures 7 and 8, it was impossible to determine

which isomer was produced.

Normally, the substitution pattern is identified by two

bands in IR spectrum, the stronger absorption bands are below

900 cm1• These out-of-plane bending and ring puckering bands

are very intense. The overtone and combination bands at 2000­

1600 cm1 are also useful. Unfortunately, this type of band

analysis is suitable only for simple aromatic ring systems.

For complicated aromatic compounds, these two areas cannot

offer reliable identification. D Using a high resolution

instrument and relatively pure samples, the C-Br stretch will

appear at 690-515 em-I, but cannot be observed with most

instruments. 24

"

20

The product obtained from bromination of benzyl

sesquixanthene could not be identified by its IR spectrum, but

could be identified by the Bielstein test. 2S The green flame

indicated that bromination had occurred. When the same method

was applied to the bromination of sesquixanthyl fluoroborate,

the Bielstein test was negative, even though the reactant

changed color. Neither the IR (IR Figure 15) nor chemical

tests could prove that a reaction had occurred.

Since a better synthesis method to brominate benzyl

sesquixanthene could not be find, we tried to nitrate benzyl

and butyl sesquixanthenes. We utilized a mixture of three

parts nitric acid and one part sUlfuric acid. At room

temperature, benzyl sesquixanthene dissolved instantly, but

the product became pitch like at about 80De. What substitute

was formed is unknown. After this procedure failed to give the

desired product, we tried concentrated nitric acid. It seems

that nitration in cold nitric acid was very slow, even after

twenty hours. In hot nitric acid benzyl sesquixanthene

dissolved faster and a reaction occurred. The product obtained

from nitration was also green. After neutralization and

filtration, the cotton-like product was analyzed by IR. From

the IR spectrum shown in Figure 14, there was no stretching

peak at 1600-1500 cm-I and 1300-1250 cm-I • Around 3447 cm-I ,

there is a large peak, which represents the 0-8 stretch. Since

these peaks are all located within the area of aromatic

absorption, we cannot be sure whether nitration was successful

21

or not.

Nitration of benzyl sesquixanthene was not successful.

From the IR spectrum, Figure 10, we can see that two peaks

appear at 3406 and 3476 em-I, and it doesn't show CSp2_B stretch

in the range 3000-2900 cml• Obviously, the protecting group

was too weak to withstand oxidation by nitric acid.

Oxidation of benzyl sesquixanthene with potassium

permanganate was difficult. Basic, neutral, and acidic

reaction conditions were attempted, and different ratios of

potassium permanganate to benzyl sesquixanthene were tried.

Generally, oxidation by potassium permanganate occurs rapidly

in basic solution. Treatment with potassium permanganate in

basic solution failed. Boiling for twenty-four hours in

neutral solution also failed. Although potassium permanganate

will slowly decompose in acidic conditions, its high oxidation

ability was critical in this reaction. oxidation occurred

after sUlfuric acid was added and the reaction occurred very

rapidly. According to IR Figure 19, the wide peak at 3500 em-I

may be due to moisture. The peak at 3081 em-I was aromatic C-B

stretch. The aromatic absorption peak at 1600.8 cm- l was

smaller. Since the IR spectrum shows methylene CSp3-B stretch,

there are two possibilities. One is that the sample was not

pure enough, the other was that it was not cleaved by

oxidation. In the IR spectrum, the aromatic major

characteristic peak 1600 cml was less intense. Other peaks,

such as 1464 and 1047 cm- l were unchanged. c-o-c absorption at

"

22

1267 cm-1 was also present.

The oxidation product was barely soluble in non-polar

organic solvents, however these product did dissolved in

common NMR solvent after several days. Although several

solutions were prepared for NMR analysis, none of these gave

satisfactory results because they were too dilute.

sesquixanthyl fluoroborate seemed easier to nitrate.

Although neither IR and NKR spectrums can distinctly indicate

that the -HOz function group was present, we can say that

nitration was successful. This conclusion is based upon both

the iron (II) hydroxide testZ6 and the sodium fusion testZ7 ,

both showing positive reSUlts. Further, the product after

nitration showed more intense fluorescence than the un­

nitrated material.

The reaction to reduce -NOz to -NHz was unsuccessful,

although the color of the product after reduction changed from

yellow to orange and to reddish orange. Neither the IR, NMR

spectrum, nor chemical tests indicated success. There was no

evidence of a color change caused by the SUbstituting amino

group. If -NHz was successfully attached on the aromatic ring,

it would be expected to be mostly meta substitution because of

-0- group attached at both ortho position. If an amino group

occupies the meta position, the compound would not show a

color change. Z8

"

23

CONCLUSION

synthesis of a bromine-substituted sesquixanthene was

successful. In the bromination reaction, the sesquixanthene

whose central carbon was protected showed better results in

terms of higher yield and fluorescence than those whose

central carbon was not protected. But in cleavage of the

protective group, an improved oxidation method needs to be

developed.

synthesizing nitro-substituted sesquixanthene was also

successful. This succeeded whether or not the molecule's

central carbon was well-protected. Nitro-sesquixanthene has

high fluorescence and high solubility in both polar and

nonpolar solvents.

24

REFERENCES

1. Lund, H., J. Am. Chem. Soc. 49, 1346, 1927.

2. Bunikiene, L.; Ramanauskas, E., Chem. Abstr. 69, 113233W, 1969.

3. Liu, Shaopu and Liu, zhongfang, Fenxi Huaxue, 10, 464, 1982; Chem. Abstr. 97, 229295, 1982.

4. Dobkina, B. M.; ZUbynina, K. B.; Nadezhdina, G. B., Khim. Metody Anal. Niobiya Splavov Ego Osn. 58, 1970.

5. prabhu, B. N.; Khopkar, S. M., Talanta, 25, 109, 1978.

6. Kuznetsov, V. I.; Kleschel'skaya, E. I., Agrokhimiya (2), 148, 1970, Chem. Abstr. 73, 41531z, 1970.

7. Badischi Anilin' soda-Fabrik A.-G. (by H. Finkenauer; H. Ottervach) British Patent 902110, 1972; Chem. Abstr. 57, p12664b. 1962.

8. Antropov. L. I.; Kozlob, E. I.; Barmachenko. I. B., Chem. Abstr. 82, 46714g, 1975.

9. Soares, V. M.; Rodrigues, R. A., Chem. Abstr. 94, 76101, 1981.

10. Brazier, J. N.; stephen, W. I., Analytica Chimica Acta 33, 625, 1965.

11. Rao, N. V.; Dutt, V. V., Chem. Abstr. 74, 105686v, 150688X, 1971.

12. Coulter, A. K.; Schuster, I. I.; Kurland, R. J. J. Am. Chem.Soc. 87, 2278, 1965.

13. Ohla, G. A., Angew. Chem. Int. Ed. 12, 173, 1973.

14. Theilacker, W.; Schulz, H.;Baumgarte, U. ;Drossler, H. G.; Rohde, W.; Thater, F. ; Uffmann, U., Angew. Chem. 69, 322, 1957.

15. Conant, J. B.; Sloan, A. W., J. Am. Chem. Soc. 45, 2466, 1923.

16. Neunhoeffer, 0.; Haase, H., J. Chem. Ber., 91, 1801, 1958.

"

25

17. Soares, V. M.; Rodriques, R. A., Chem. Abstr. 94, 76101, 1981.

18. Fold, V.: Hawes, J. Chem. Soc. 2102, 1951.

19. Deno, N. C.; Jaruzel, J.; Schrieseim, A. J.,J. Org. Chem. 19, 155, 1954.

20. Oldrich Valcl, M. Se.; Irena Memcova; Valelav CUk, CRC Handbook of Triatylmethane and Xanthene Dyes. 4, 291, CRC Press, Boca Raton, FL, 1981.

21. Oldrich Valel, M. Se.; Irena Memcova: Valclav Cuk, CRC Handbook of Triarymethane and Xanthene Dyes. 3, 233, CRC Press, Boca Raton, FL, 1981.

22. Vanallen J. V., J. org. Chem., 23, 1679, 1958.

23. Koji Nakanishi; Phillippa H. Solomon, Infrared Absorption Spectroscopy, 1977, page 20.

24. Douglas, C. N.; Michael P. D., J. Org. Chem. 65, 1977.

25. Williamson K. L., Macroscale and Microscale organic Experiments, D.C. Heath, Lexington, MA, 1989.

26. Williamson K. L., Macroscale and Microseale organic Experiments, D.C. Heath, Lexington, MA, 1989, page 660.

27. Williamson K. L., Macroscale and Microscale organic Experiments, D.C. Heath, Lexington, MA, 1989, page 649.

28. Lucas J.; Pressman D, principles and Practice in organic Chemistry, wiley, New York, 1949, page 429.

29. Slocum, D.W., and Jennings, C.A. J. Org. Chem. 14, 3653, 1976.

,,"~,~

f'll" . 1~11fi'

'111' :l

l·~

26

Figure 1: IR spectrum of 2,6,2',6',2",6"­

hexamethoxytriphenylcarbinol

(KBr pellet)

I -----,---­ I -----, I

3000 2000 1000 WavenuITlbers (crn-l)

......-l C";)

C'­

W­

r­ee co

c::. ~ o oc:l_­

c:o t:O ~OC\l _

......-l .....-l

1c:"'J

~ f'I:O

~~ ......-l......-l

Res= 2 cln-lIR spectrum No.1

200

Q) (J

~ ro

l;")

+oJ

.1100

I N '-0 Q')C,\l

0)1 ......-l

c:\l C'-:J'-0 .""

~-• l;") ~CO

~

c:"'JC\2C' N

I 0

2,6,2' .6' .2" .6" - hexarnethoxytriphenylcarbinolL--___ .. _

t '" ~tll

lIJ~'I>. . ilr,l ~'jl~

"l~1

1'1

:~,. I'" j

"h

'.I'

27

Fiqure 2: IR spectrum of 9-(2,6-dimethoxyphenyl)-1,8­

dimethoxyxanthydrol

(KBr pellet)

l:'­

c:'\l o c:o

'"Eb

~ ~

I I

--I

l:'­--I rn

I

1000

­C\l •

~-

~

co C"j-I I

~ - f'.. ~ c:o ~ C\l co f'.co ~ N

--I --I -Res= 2 clll.-1

I

2000 Wavenurnbers (cnl.-l)

C'J • I

M I ~m-.,.....fC\.rt' •

C'?co ~t:":l C\lr:o

r:\l

I

3000

~

--I o ~

r.;>J

U')

C\l o lr.l C":l

9--(2.6--diIllethoxyphenyl)--1,B-diuH:·thoxyxanthydrol

Ir spectrulU No.2

0­

50

100

Q) CJ ~ «S

+J ....,J..... Ei (Jl

~ cd ~ ~

:£ eXn.6~4toxpAq~u.x~nbs.s ~O mnx~oeds UI

Tra

nsm

itta

nce

0 a.

0

~

0 0

i "~

UJ

I'C

r:ll ~

~

~,

~ ~

~

~

~ ::r ~ p. ., 0 """'"

~

~

til

"'0 ro r)

f"'"

"'$

~ S

2 0 , W

~

0 0 0

3496

.7 -

3406

.1 -

~

~

til II N

I":i S I P-'

~

)I)

~

I'C =' ~ S ~N

I'C

0

""I

0 tn

0 -(j S I

~

'-'

1618

.2

1485

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1272

-13

4

~

0 0 0 1~2ttt~~6

_

746.

4 -

580.

5

Ell

••PI,,,, I'':;

'li,"1 I:l~

If

':~ .II

, ..;!~

. " i ' I

29

Figure 4: IR spectrum of fluroboric sesquixanthene

(KBr pellet)

200

lD

co Q.) C» (;) o

C"':l~ .s 100 ~ • .-4

S (fJ

~ a:I

~

I I 'I If' ­o ,~ l'-~ C"':l

lQM ceo• Lr:> ~ o~~ .....fI­ccC\l ~co U":I~ c:o <:0O':'......-i ll.l~ .,....ri U":I

~ o....... "" -­ -

2000 1000 Wavenurnbers (crn.-1)

IR spectrull:.l. No.4 Res= 2 clTI-l

f'luroboric Sesquixanthene

3000

I

"I 1i

(~etted .za)l)

eueq~uvxlnbses tAZUea ~O mn.z~geds HI

DE

I

--

~ttl

~

ro ~

(IJ'N

~

<'ll

I~

('j

(+rJ

) 11

ro C!J

~

w~

"'" ::l

0~

~.

0

Z~

0

0~

.

I~

01

iJ'

~

ro ~

~

=:l <'ll

<1

lro

Ul

ctI

I II

::l I

~

I

N

S ,:'

jI

c'~

s C1

l 0

11

0I

til

0I

I­

I -(':I

I S

I I ......

I I I I I I­

I 0

! 0

i 0

! I

Tra

nsm

itta

nce

N

0

0

II II

3025

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-

1614

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1460

-

1266

.2 -

101~§4~6

-

I 77

3.4

-I

700.

1 -

I L

630.

7 - 54

9.7

-

I I I I

Tra

nsm

itta

nce ro

0

0

ttl ~

~

~ ~

"<:

l-'

r.tJ

"0

(D

IJ2

0 ib

00

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~

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""",

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I:..:J 0

3072

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~ ~

~

Z

0

0 0 29

62.

-

2859

.3

-("

'I' =r

Cl:l

(D

~

~ ~

~

ib

(l

r.IJ

-< (!l

II ~

~

N

S

':" S

0'

<tI , r" 0

I ,... ~ -. <':l

g I

a I 16

12.4

-)«

­ -14~~2-

-

1267

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13.5

1Q64

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0

797.

5 -

742.

5 -

32

~ ,!

",' ~,

'~" , lSIl'1~~"1

Ilrt il~',' 11,; III'",~.

',12', ;,: ':;"!

Figure 7: XR spectrum of the product obtained

bromination of benzyl sesquixanthene

(KBr pellet)

from the

l\J,,: 1 1'_:1

,,: :i'''~1

:~ iWi;

I:! J'II'.;<

w

,I t' I, II' I~ ~, jl: I

f~"

Tra

nsnl

itta

nce

0 lo

­

0 N

0

~

0

ttl

~

""'"' ~

~

r.JJ

N ~

~

~ -0 ("

'l" ~

"'l

"1..

~

Cf

S"1

0 a

z 0

0 r:tJ

-..

] ~

1$ ~

~

(D

.... al

~ ~

II

~ '*

N

=r '"

('C

• ~

~

('C

I """

c,.:l 0 0 0

:;;J

~ < (tJ D

~ S

a'N

(tJ

0

~ 0 0

,­

3085

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-

2951

.9

-28

68

-

~ ::l ~ I 10­ -­

14~~O%.i

_

1599

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1269

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2

10­

0 0 0

1052

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-

869.

8 77

3.4

- 701.

-

-

33

~!.!.. ~: ,~" l QJl~~!'io

ti Figure 8: IR spectrum of product obtained from the lr:~""

:'~':: ij,-,,,,,Ii! bromination of butyl sesquixanthene~:'~2":i!,L I~:

~~il~ (KBr pellet)'::~r,~

il~' f~i~ i~li!

I: 'gl~ I :~~

1 11 ".

J .',"

;:: ~~I : ,,.JIll,!

I:'~I':

Tra

nsn1

ittan

ce

N

0 0

IJj ~

~

;:::l

~

r:JJ'-<:

~

.­\D

~

<":

> '1

~

.....

"'i

~

="'l

S

~0

08

z 0

0 0

00

0 It

.

00

co

~

~

I~

~

~

,

.....

I~

~

-<

Po'

r.tJ

(U

~

II ~

~

~

=:"

N

S

It

=:s

(~

O'"

N..

It

~

I'D

0 I

~ 0

~

0 -­ ~ a I 15

96

-~

-­l!tal~

-­12

75.8

-

I-'

1050

.2 -

1115

.8 -

0 0 0 87

2. '7

-77

3.4

-

622

-

I

'--­

J

34

\.. ~~r,rl

.....w,:'1 Figure 9: IR spectrum of the product obtained from the

!~.~: ~~ oxidation of benzyl trinitrosesquixanthene'~~

' • I~;"'J' (KBr pellet),JllP'li~

,(1II 'ilflil

II~

!~ ~~: I~ )"1'".,. ~' ",-,

~;~ f!~

--~

I

IN o "<:t4(.....

C\l ['"­t-

ex:::> 0)

CO CO

1000

o::J

o o c:o -­

Res= 2 crn-l

2000 Wavenurnbers (crn-l)

t>:I

o CO CO C\l

......... -­CO o C":l

3000

IR spectruIU No.9

3,3' ,3"--Tribrcnnosesquixanthene

0-1

I I ...-j4

.....-i

eJM~ C":l

~ r-­ l'­

~~ "<:t4 0

........ .....-i .....-i

<:t>(.) 90 ~ ...., ~ ~

+-> .~

S rn Q CO ~

E-<

35

i

~~ , ,~'l~~ '~,.,

'1"11 tl'~:I~:

~r"~~

:1:~~I

I

I~.~~".~.': j~ -~.I~ ·~I ;~~: ~.~~:

~,

t~ ~~; ~~~

~

Figure 10: IR spectrum of the product obtained from the

nitration of fluoroboric

(KBr pellet)

sesquixanthene

--

0

~

~

~ 0 ~ I~ ....

(1

~

I~. ::l ....

~

0 ~

[,(] t'tI [Jl

~ ~

....

~

~ ::l c-+­ =r

t'tI :::l en

~

~

00 ~

~

(';J

r+

~

~ S

Z

0 . ~ 0 ::0

~

00 II N

(') S

I ~

~

~ <1 \tI ~

~

=

0­ \tI -~

00

(';J S

I ""'"

Tra

nsm

itta

nce lV

....

00

~

0 0 0

3054

.1

-

N

0 0 0 ~

0 0 0

I

1633

.B

-15

49.7

-

1465

.8 -

1338

.5 - 12

59.4

- 1164

1~

.'Z5

--

784

-

559.

3 -

-

36

Fiqure 11: IR spectrum of the product obtained from the

reduction of fluoroboric tribromosesquixanthene

(KBr pellet)

C":J

o:l .0 lQ

q ~ """-'I.

tC:l CO l'­

l,Q.'l--I

~ ~

C\} co-

1000

~

0:>

l:'-:I 'lQo IN lD C7J ...... lD • "......ll ~

~ a:JC"':l ..0­~ '"i" ......

-.t'

~ f;'? ~ -­

2000 Wavenunl.bers (CIll- 1)

3000

IR spectruIll No.ll Res= 2 cln-l

Reduction of fluoroboric trinitrosesquixanthene

o

30 -I At" I. ~

20

v Q

~ ~ ~

+-'..... S 10

r-­rn 1:::1

~e to 0Eo-< C'j

37

~1

I ~ ';;+0'

it' Figure 12: IR spectrum of the product obtained from the

nitration of butyl sesquixanthene

(KBr pellet)

i

3091

.7 ­

2964

.4­

-

559.

3 ---

-----=

1

Tra

nsn1

ittan

ce

o

C,.:I o o o ~ o a o -

38

'1.,1~r:'~.~l,tl' Figure 13: IR spectrum of the product obtained from ~:~:' :: r the reduction of butyl sesquixanthene~< :1

(KBr pellet)~.~l !r,.~".

..Ot.f -

IR spectrum No.13 Res= 2 cln-l

The product of butyl sesquixanthene nitration reduction

-I

C":l 0')

..0 U')

C:l C\l .....-l 0:>

C:O' ;.I

t:O ~

~ ~ o -­

1000

COI~

~ I ~c» - I cO-~lO

ll? C"1Y.l N ~co.....t:t4......-i

lQ aD "'" .,.......jc:.o -­

~ .,.......j

..0

~ C'? co-

I I

2000 Wavenurnbers (crn-i)

c:J C\l co o C':l

3000

o

40

Q.I e..;, c:: ~ 20 ~-­S ct:l t:1 ro h

Eo-<

40

Figure 15: IR spectrum of the product obtained from the

bromination of fluoroboric

sesquixanthene

(KBr pellet)

Tra

nsm

itta

nce

ro ~

0

0 0

-~ -~

~

0

1'.ll

11

0 0'

~

(0

('j

0 11 ~

11

~

~.

('j

S ~

0

3054

.1

-~

.., .... 0­ ., 0 S

'Z

0 . ,... C,i1

~

0 0

0

1

00

I<'C 00

~

('D

1'.ll II

~ <: ('U D

,Q

~

~ ....

('~

S i'<

~

D

~ ::r

('j S I 10"""

0'"

t-J

('U

0 ~

0 -0 <Ii

:= <Ii

0 S I 16

36.5

-~ -

1550

.7 -

1465

.8 -

1338

.5

- 1259

.4 - 1164

-

~

0 10

~~?P

'§ -

0 0

ftat9

­-

559.

3 -

41

Figure 16. NMR spectrum of the solvent CDC1

3

Reference: TMS

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IIlFUlNC£ : -~. I SOLVlNT : ~ _

CONC: -----------.----------i AIlPlITUD£ : SPlClIIUIi : 1 __ . _ 'NllGllAl . _

'H SP£C fllUIl NO. :

SAIIPU : _Jl~tb.loul.lonL _

----_ ......... . 'llfU ... : I

'.,., J

SWUP Tllll: DllDO/I 'OUC 0

1;"

I 1030 1.0•• ••• •p - O....n. (CH, I, SO (CH,I,CO C'eloh.....

CH.OH CH,P"

40'0­",0•CH.C'.

NH Im,dn

10

I-- C. Cit, 1'---­ I I -CH, CO +- - CH'-cr' - CH.-St+­I -CH,O-­ ----~H.C.,.C

HC - eH I - CH, A. -II -CH.N-­

- C CH,O--C CH, ,. - ~- C CH, C ....""'... -­ CCH,O­ I -CCH,N­ -CH•...• -", CH. 0­ - ~C CH,C-­

I -·CCH. OJ­ -HC:C

-A.CH,N-­ I .....tlGI IIH

7010'0 • • •f-I '.3 ".CF,COOH P"id,n.I.1 P,.id,no" I ';IridiMlIII C. •.CHC'.

10.0

r

HITACHI PERt<IN ELM!:R CHAII' NO.•~,.aa ~J'.~

42

Fiqure 17: NMR spectrum of deuterated acetone

Reference: TMS

, .

----I-- CHO ~ ~ :

"" : A_lie 'itt

• • •1-, l.:t ,-.C',COOH p,.idinel.1 P,'id.... ' ~ I Pjl'idintl,1lC, ,.CHCI,

A,·H

2

I SEC

OPER,,'OR:

.wnl' flIIE: I!I :t001l SOSEC 0

DATE: 04/15/9]

CH'" NO.'~J.aa ~".~

H. lEvn :

11111".115 :

I .. 1-' i 'il lULl Ito LEVEL: _

CAIN:

swnl' WIDTH:

I .:-:l!!1--- l!!!l-'" 1:J

c..---r .!I-J

lIE, EIlENCE : _.!"S I SOLYEN' : ~ _ CONC: . __ . _

AlIl'LnUOE : 1] snC'RUII: ~

INTEGRAL'

SAIIPLE : __~=!'_~~!~!... _

'H SPECnUll NO. :

----_ ....... . F1UE"e&iwh:-=]

t·· :.IS

- CH,'SIT­

10]040so­ ",,0•CH,Cr,

10

HITACHI PERMIN ELMI!R

10••• •(CH,', SO (CH, ,,CO C'cloht..... CH,PIl

CzCH,--­ - CH,COT - CH,-C-.-­I -CH,O-­ ----.:H,C~C HC - Cit -----+--­ I - CH,A, -I

I -CH,H-­-C-CH,O--CCH,"'­ ~_CCH'C]m;""',,,

-­ CCH.O­ I -CCH,H­ -CH, -'I<CH,O­ -~CCH,C--

I -·C CH, N­ -ItC;C ....idn -A, CH,-N-­ I ....ino

HH-­ I - IIH

7010'010_0

r

43

Figure 18: NMR spectrum of 9-(2,6-dimethoxyphenyl)-1,8­

dimethoxyxanthydrol

Solvent: CDC13

Reference: THS

..

.'

SIC

04/15/9JDATl :

OPlRATOR:

aWup TllIl: 11300/1 10UC 0

",Lun: _ CAIN:

--­_......• II •

FILTER HI; I l:l!I:n!IOI _ OJ

l1li1 SWl: ':ID~~i~ ·ITJ

I i II I its... ­ '1I j i:J

~•II I::tIt

II

H,LEvn:

REFlRlNCl : -~ I SOLVENT: JlCJ:.L, .......; CONC: _ _

AIiPLITUDl : SPlCTAUN: .l1 ~

INTlGAAl'

1'II.rll'lllALJ

NH ,m,61.

II ,.I A!IIU.S :

s C, ,.CHCI, CH,Ph

I A,H I C=CH'-I-­ - CH,COT - CN"C1 -CH,-CH,O-­ ----.:H,C~C

He - CH I - CH, fI, -II -CH N-­

--C-CH,O--CCH",---=­ ~-CCH'C be - CCH;O­ I --CCH,H-­ -CH, fm IS -~. CH, 0­ - =C CH,C-­

I -"C C11, 11­ -Ite;c - Ar CHI N-­ I Imlf'O

I IIHAI: A_tie: " ••

'00

'H SPECTRUM N~ : )

S~NPlE : _

9-12.6-dl~~tho.yhpenyll

1.8-dl~~tho.y.anthydrol

90 80 70 60 10 40 , 0 1.0 10. .. . - .... II "'.CF,COOHp"id.n.(.' P"Nlinll ,I Pjl'i41inel'I CH,C', 11,0 ICH, ),50 (CH,I,CO C'clah.....

HITACHI PERt<lN ELM~R CNa., "0....,_ l7D(u'08

44

Fiqure 19: NMR spectrum of sesquixanthydrol

Solvent: CDC~

Reference: TMS

. '

I

LiLl...!lI...J

H, LEVU:

I " I. i UL:l_iAl

IWU' WIDT":

• iT."". .HI 'T' i ]----_ ....... .

t'·T.5

II I m~~:~':'::_~"_1

AII'LITUDI : I'ICTIIUM : .1.l .. _ I"TEGllAl . H _

• , ,CH,-StT-

No LUll: _

CAl" :

II

• II ~O_

10.0 10 70 10 40 3 a 1.0 1.0'0 • • • • •• ••• •1-11.3 ".Cr.COOH P,.idin.I.1 p,.idine" I P'......"I CH,C'. 11,0 '-O....n. (CH.I.50 (CH.I,CO C'elo/l...... CoH•.CHCI. CH.OH CH,pIl

t- -, I I .A.H c. CH.---- - CH, CO, - CH,-C-:-r- ­-+-CHO -CH,O-- ----.:H,C-C1

HC - eH I - CH, A'-I-CH N-­-C CH,O--C CH, ~ • ...:.... ~-C CH, C-r.:"_mbe I

-- C(H;O- -CCH,N- -CH,·il"""I - A. eH. 0- - ~CCH,C--

-~CCH,,,- -HGC _idn -A.CH,·N-- tonino

'" : '-lie .ift NH-- I IfH

HfTACHI PERI<IN ~eA

I I

'H 5PlCTRuM NO. : ,

SAMPLE: ..5uquLulltheu__

flLUII III: I llILllI!IT:::J

IWU' TlIII: 11300/IS0nc 0 '~C DAU: 05/01")

OplRATOII :

IIfllAlIllS :

CMllt 1m, ...,_ S7'I1(' ••.,

45

Figure 20: NMR spectrum of benzyl sesquixanthene

Solvent: CDC~

Reference: THS

. '

A, M­-4-CHO I I

AI: "-lie ,...

05/04/9)

CNallT 110.'.,_ J71YJO ••~

DATE:

OPlR"TOR:

IIUI"-" :

r7 JT::I T I I I J T­---_......• II •

'IL TUI ... : II lbLL"I.J

IWUP TillE: 113OO/l505(C 0 I SIC

H, LEvn : 1 S'lIM:

I LITTI!lJ

SWUP WIDTH:-- --""

t· TU ::-t - CN,'It;-­

104050­11,0

SAIIPLE : •

I • I. I llLiDLJ

'H SPEC TRUll NO.: 5

Benoyl Selqul •• nthene

UFUlNCE : __ nts I SOLVENT: __ • __ .Da:.l,.. _ COMC : ._ ..... ' , ... _

AMPLITUDE : SPlCTRUll: 11

INTEGllAl . ::::..:~~~~:~:==

N.LEVEl :

•CH,CI,

HITACHI PERKIN ELM!!'"

10 ] 0 z.o••• •ICH,I, SO (CHoI,CO C'elah...... CH,P"

C· CH, --­ - CIl, CO T - CH,-C­..--. I -CH,O­ --':H'CJ~

HC - CII -----l..­ I - CH, AI -I -CI1,N-­I --CCH.O--CCH,·~I- ~-CCH'C ""mb...

CCH,O­ I -CCH,N­ -CH, - A. CH, 0­ -:C CH,C-­

I -~CCH. N­ -IlCoC

NH ,mid.. - Ar 1"' M-­ I NH ,mlllO

70

II

10

'.

to • • •1-11.3 ' ••C' ,COOH P"id.n.f.1 P"id'Ilf' rI Pjl'i4lilttf'"C, ,.CHCI,

100

rT'

SAMPLE: __ . __ • __ ••__ • _

'H SPECTRUII NO.: 5

SIC

0510419]

CHIIT 110....,_ ~,.•••

DATE:

OPERATOR:

II

RElla-liS:

r·. _---y0...-_. , .. J JaLJI

H,LEYU:

REFERENCE: _ llIS I SOLVENT: _._._.Da:l,... CONC: .. ..... " ... _

AIIPlITUDE : SPlCTRUM: .... .!.~_._. _ IHTEGUl . __ ._.~_ •• _

_.... _......• I' • flL TER HI: II

c:nLtJIIIlI. :J

SWUP TillE: 1l300/150UC 0

'"nayl S••qul.anth.nl

H, LEYU : .... ._

U'N:

I ULIi!lJ

SWUP WIDT":

I ,-;,..... let.,. , L:J

t·· T.S

::-I - CH"St;­

10

l!

]04050­H,O•CH,CI,

60

I

70

II

10'0 • • •l-11.3".Cf.COOHp,,;d,n.C.1 P"id,nt'11 Pjl'ilI"","C, ,.CHCI,

A, H

. •• zI r .~o.,.~·· 0 C'CH I (eH·

_ l "' ~ ~~, I I <~.. ,I," ',",I" •'" ------"-­ I '",..' <"......

I -ICH,O -­ - CH, CO.!... ...

I ' - ,",'< ., . ~ - '" .--.:~..c ..,. -­ CCH O-CCH 0­ -ell H''''-.I H,C~C,I -". eH 0' - I' CCIl",,"':"­,_ -C -_......' I -.:""< ,",'­ ~ C ~H, C~_", CH N ·e eH. H. CH.·il"."mb...

I' -­ -lIe;c bNH·m,no J I

HITACHI PERK IIN ELM!!'R

100

46

Figure 21: N.MR spectrum of butyl sesquixanthene

Solvent: CDCl3

Reference: TMS

SIC

--­

05104/9 )

OPERATOR:

DATE :

REMARkS:

CHAR' MO. 1"'_ .C7.".,~

SWEEP WIDTH: ... "'" ........

H, LEVEL:

[2! 1·'.-1

I -. I.A I , ... LiAI j

H.LEVEL:

lOAIN:

CIAr:r:r r::r J.-J....­-,. ....• •• • fiLTER Ib: X

I CiG r ;0. I =:J

SWEEP TIME: C1300/150SEC 0 1

REfERENCE: THS I SOLVENT: DCCl, CONC : .. _

AMPLITUDE: SPECTRUM: L __. _ INTEGRAL: _

SAMPLE: _._. __

'H SPECTRUM NO.: 6

Butyl lesquixlnthene

Ib

II

~.. TIIS ~

·St"":'""- CH,

\.03.0

T'

4.0

HITACHI PERKIN ELMER

5.0­",0

Z.O•• ••• •p-D"u.I (CH,I,SO (CH,I,CO C,c/oll.u•• CH,OH tH,Pft

I I -CH,'COT - CH,·C.....!.I -,CH,O­ -I-':H'CUJ--­ - CH."A, --tH N-­I -ttH.O--C·CH,·_,~ --C·CH,·C

-­ CCH,O­ I -CCH.N-­ ~ -CH, m,mblll - AI CH, 0­ - -C CH,C-­

I --CCH,H­ -HC:C -A,CH ·N-­ II t NH ,m,na

•CH,C',

HH ",ud"

'.0

I

AJ : AP'CIMtlC IIftl

10.0 '.0 '.0 7.0• • •I 1.3 ".Cf,COOH P,ridi.,C.I P,rid;."71 P,ridMteI"IC,H•.CHCI,

Ar'H C· CH,-....;-------11 I HC • eH _

'1'

47

Figure 22: HMR spectrum of the product obtained from the

bromination of benzyl sesquixanthene

Solvent: Deuterated acetone

Reference: TMS

"-Ttill Il" j "J H. LEVU:

SIC

OVI~/lJ

OPERA TOil :

DATI:

IlfllA1l1lS :

H, LEVEL: •

SAIN:

SWU, WIOT":

I .-:-t"'. /!!!it", L:J

~

UnRINCE : __~ _ SOLVENT: =, _ CONC: ----------------------1 AII'L1 TUDE : SPECTIlUII: ~~ _ INTEGIlAl' _­ L _

'H SPECnUM HO I

SAMPLE ~ ----------n-------1

-_ .• •• • 'IL T[II HI; _

tDLI:!!!KI __ ]

SWU, TIllE: .3OO/15051t 0 1

'en.yl trlbrOGlo

8eequlManthene

t· TU

::-I - CH,'St;­

10

II

•

10.0 to 10 70 60

a.· a.....hC Il~.

""-'LH' ,=»ERMfN ELMI!R CHal' 110.••r_ T7"''''06

48

Figure 23: NMR spectrum of the product obtained from the

nitration of fluoroboric sesquixanthene

Solvent: Deuterated acetone

Reference: THS

---l--CHO' I A,·H

AI: __lie ,oe,

•

1 SIC

05/01l/9)

II!IIAIlIIS :

DATE :

OPIIIATOII ;

CMlII' lID. 4.'_ J7'V".~

... LEVEL: ._ .. __

5AI" : c-Ul!llJ

III.UINCE : __.!!!~

~:~~~N.~~~~~~~_~._.~ AIIPLITUDE : SPICTRUII: . U •• __ ._. _ INTEGIIAl : .... !_~_.._. _

",LEVU:

.1. ...... JLiLl

IWIIP WIDTN:-- --""

SAIIPLE : • .._. __

Fluoroborlc Trlnllro· •••qul ••nthene

'H SPECTIIUM NO. :

[ I I.-------rT rJ":J I:J-_ .. .. . 'llTlIt~_:::J

IWUP TIllE: 1)300/IS0SEC 0

t·· 'liS

-1.0

II

]0 1.0•• ••• •p-O....n. ICH,I.50 ICH,I.CO C'clo/l...... CH.OH CH.P~

40

..

50­H,O•CHIC'.

HITACHI P£R~IN ELMER

.0

I---- C· CH·­I '-­ I I -CH, COT - CH'-C

J ' -CH,-St+­I -CH.O-­ ----.:H,CkC

HC . eH I -CH, A, -/

I -CH,N-­- C CH,O--C CH, ,,­ ~- C CH, C mb

-­ C CH,O­ I --C CH, H-­ - CH, "" tiS - ,II, CH, 0­ - =C CH,C-­

I --eCH,N­ -HCoC ,mldl, -A,CH."H-­ I ,mino

NH -­ I IIH

m I

'.0 10 70• • •!-1l.J'••Cf,COOHp"id;n.I.1 P"idi.... )) Pil'....'''. C. ,.CHe',

10.0

I

I, YILIN QIAO , hereby submit this thesis to Emporia

state University as partial fulfillment of the requirements

for an advanced degree. I agree that the library of the

University may make it available for use in accordance with

its regulations governing materials of this type. I further

agree that quoting, photocopying, or other reproduction of

this document os allowed for private study, scholarship

(including teaching) and research purposes of a nonprofit

nature. No copying which involves potential financial gain

will be allowed without written permission of the author.

LLf/;i/} 0 laD Signature of Author

September 1st, 1994 Date