Pseudo-atom-molecular orbital approach to substituent effects in

Pseudo-atom-molecular orbital approach to substituent effects in organic compounds. I. Spin-spin coupling in substituted methanes. Gary E. Maciel, and...
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520 Table 11. Partial Degradation of Pyridoxol Derived from [I-14C]Glucose

4’ A

~

~

,

~

~

Product (C atoms of pyridoxol)

5’

CH20H A

2’

A

A

Figure 1. The distribution of label in pyridoxol. Sites of activity derived from [I-’4C]glycerol (triangles) (relative specific activity -20 %) and from [2-14C]glycerol(circles) (relative specific activity -3373, demonstrated by degradation (A,0 ) (Table I) or inferred (A, 0).

radiocarbon. The pattern of labeling observed within glycerol-derived pyridoxol (Figure 1) is exactly as predicted by, and therefore supports, the hypothesis outlined in Scheme I. Table I. Observed and Predicted Distribution of Activity within Pyridoxol Derived from [14C]Glycerol

Product (C atcms of pyridoxol) Pyridoxol (all) Scheme 11, sequence a 3-0-Methylpyridoxol (2) (all) Dicarboxvlic acid (3) (ani Monocarboxylic acid (4) (all but C-4’) :. c - 4 ’ Scheme 111 Phenylcarbinol (6) (all) Benzoic acid (C-5’) Scheme 11, sequence b Acetic acid (C-2’,2) Methylamine (C-2’) Scheme 11, sequence c 2,4-Dimethylpyridine derivative 5 (all) Acetic acid (C-2’,4 ’,2,4) Methylamine (C-2’,4’)

Re1 spec act. (%) (pyridoxol = 100) of the product derived from [l-14C]Glycerol [2-14C]Glycerol Obsd Calcd Obsd Calcd 100 i 3

100

100 I

100

3

Scheme 11, sequence a 3-0-Methylpyridoxol (2) (all) Dicarboxylic acid (3) (all) Monocarboxylic acid (4) (all but C-4’) :. c - 4 ’

2

100

Product (C atoms of pyridoxol)

100

k

3

100

78

=k

2

80

22 i 2

20

98 i 2

100

Pyridoxol (all) Scheme 11, sequence b Acetic acid (C-2’,2) Scheme 11, sequence c 2,4-Dimethylpyridine derivative 5 (all) Acetic acid (C-2’,4’,2,4)

0

0 99 f 5

0.5

100 0.2

0

35 i- 1 2.4 0.4

+

33 0

100

101 & 4

100

22 i. 1

20

32 i 1

33

19 f 1

20

1

20

22 =k 1 18 =t 1

20 20

98 i 1

22

=t

2k

A further experiment, with [I-14C]glucose (0.5 mCi; Amersham/Searle) as the sole carbon source, was intended to throw light on the mode of incorporation of triose phosphate. Glycolytic breakdown of [ I - 14C]glucose leads to in situ formation of [I-’4C]dihydroxyacetone 1-phosphate and thence of [3-14C]~-glyceraldehyde 3-phosphate. According to Scheme I, label from the latter should enter C-5’ and, aiu pyruvate and acetaldehyde, C-2’ of pyridoxol. Activity from the former might be found either at C-3 or at C-4’, depending on the mode of the postulated combination of acetaldehyde with phosphodihydroxyacetone, leading to the intermediacy of the 3-phosphate or the 1-phosphate, respectively, of 5-deoxy-~-xylulose. Decarboxylation of the dicarboxylic acid (3) obtained from the [ 14C]glucose-derived pyridoxol gave the mono-

100 i 5 62 i 3 38 It 4

Table 111. Partial Degradation of Pyridoxol Derived from [3-I4C]Serine

+

100

100 i 4

carboxylic acid (4) containing only 60% of the total activity (Table II), demonstrating the presence of label at C-4’. This result is consistent with the latter of the two alternatives, i.e., condensation of acetaldehyde and phosphodihydroxyacetone to form the 1-phosphate of 5-deoxy-~-xylose,jas shown in Scheme 1. In a fourth experiment, the role of serine in the biosynthesis of pyridoxo16 was explored. Pyridoxol, isolated from a culture which had been incubated with [31 4 C ] ~ ~ - ~ e (0.2 r i n emCi ; Amersham/Searle), on KuhnRoth oxidation yielded acetate (C-2’,2), containing almost the entire activity of the intact vitamin (Table 111).

99

103 i 6

Re1 spec act.

Re1 spec act. 100 i: 3 92 i 4 100 i 5 63 i 3

Since this is the labeling pattern which was observed when pyruvate serves as the precursor of pyridoxol,2 and since conversion of serine into pyruvate, a welldocumented catabolic r e a c t i ~ n ,is~ ~irre~ersible,~ ~ it follows that incorporation of serine into pyridoxol takes place cia pyruvic acid. ( 5 ) P. A . J. Gorin, L. Hough, and J. I