Cytiva com O o o o o o o o ho o o o ho ho ho ho o o o o o o o ho o o ho ho o o oh ho o ho ho sephadex



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11273 10061

CH
3
C H N
C O H
O
O
C O H
NH C C H
3
O
O
1.
2.
Fig 3. Separation of 2- and 4-acetamidobenzoic acid on Sephadex LH-20.
Column: 
Sephadex LH-20, 2.5 × 200 cm
Sample: 
Mixture of 2- and 4-acetamidobenzoic acid
Eluent: 
Acetone
Flow rate: 
8 mL/min
Detection: 
Refractive index (RI)
Yield: 
250 mg 2-acetamidobenzoic acid
254 mg 4-acetamidobenzoic acid


5
mg
30
20
10
1600
1800
mL
2000
mg
30
20
10
1600
1800
mL
2000
mg
30
20
10
1600
1800
mL
2000
mg
30
20
10
1600
1800
mL
2000
Medium:
Sephadex LH-20
Mobile phase:
Heptane-chloroform-ethanol, 20:20:1
Solute:
Budesonide 21-acetate (XVII)
Sample volumes:
(
A) 500 mg, (B) 1500 mg, (C) 3000 mg, and (D) 5000 mg
A
48
0 nm
0.8
0.6
0.4
0.2
0.0
100
80
60
40
20
0
0
5
10
15
20
Pho
spho
lipid (
nmol
)
Fraction volume (mL)
OD
PL
A
48
0 nm
1.0
0.8
0.6
0.4
0.2
0.0
0. 4
0. 3
0. 2
0. 1
0. 0
0
5
10
15
20
A
48
0 nm
(free DXR
)
Fraction volume (mL)
LT60C L-DXR batch
Free DXR
Fig 4A. Sephadex LH-20 (1 × 20 cm) elution profiles of L-DXR clinical batch 
LT4C stored at 4°C and phospholipid by modified Bartlett assay (








and A
480
(
ο

ο

ο

ο
).
Fig 5. Structure of budesonide C-22 epimer. 
Fig 6. Effect of loading with high sample mass in preparative gel 
chromatography. Amount of sample/fraction plotted against elution volume.
Fig 4B. Sephadex LH-20 (1 × 20 cm) elution profile of L-DXR clinical batch 
LT60C stored at 60°C (…



…) and free DXR (…



…). Results of the Bartlett 
assay are not shown.
Preparative separation of an epimeric 
mixture of budesonide
Attempts to resolve epimeric mixtures of steroids similar to 
budesonide by fractional crystallization have met with limited 
success. The development of a chromatographic separation 
method on Sephadex LH-20 proved to provide a more effective 
preparative method (12). As synthesized, the glucocortoid, 
budesonide, is a mixture of 1:1 of the C-22 epimer, see Figure 5. 
During the evaluation of budesonide as an inflammatory, it 
was desirable to evaluate the chemical and pharmaco-logical 
properties of the two epimers. Sephadex LH-20 was packed into 
a preparative column (6.3 × 75 cm) and different loadings of the 
epimeric mixture of budesonide were run to see the trade-off 
between resolution and loading, see Figure 6. When restricting 
the chromatography to a single cycle, sample loading at 1500 mg 
proved to be a practical preparative load.
O
CH
3
CH
2
OH
B
C O
HO
CH
3
O
O C

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