Wine Chemistry and Biochemistry

(Steven Felgate) #1

8D Yeasts and Wine Flavour 345


sulfate

sulfite

sulfide

L-cysteine homocysteine

glutathione

L-methionine

S-adenosyl-
L-methionine

O-acetyl-L-homoserine

homoserine

L-aspartate

L-serine

3-phospho-
glycerate

Met5p
Met10p

Cys3p Cys4pMet17p

sulfate sulfide

Sul1p,Sul2p

Met6p

glutathione cysteinemethionine

3 NAD(P)H

acetyl-CoA
(pantothenate)

ATP

glucose
glucose

Str2p Str3p

sulfide
+ pyruvate
+ ammonia
cysteine
desulfhyrase

Mup1p
Mup3p
Gap1p

Mup1p
Yct1p
Hgt1,Opt1p Gap1p

cysta-
thionine
α-keto-
γ-(methylthio)-
butyrate
methional

methanethiol methionol

methanethioacetate

demethiolase

transaminase
CO 2
Adh1p

Ydr380wp

threonine

NH 3 NADH

acetyl-CoA Atf1p?

acetaldehyde
or ethanol

ethanethiol

ethanethio-
acetate

acetyl-CoA Atf1p?

sulfide?

ATP
ATP
a thio-
redoxin

sulfite

Ssu1p

Fig. 8D.8Sulfur metabolism inSaccharomyces cerevisiaeyeast
Cysteine and methionine are accumulated by general and specific permeases (Mup1p, Mup3p,
Gap1p, Yct1p) according to nutrient composition of must, but typically low concentrations
cause early induction of the sulfate assimilation pathway. Sulfate is actively accumulated (Sul1p,
Sul2p) and reduced to sulfite, which is then reduced to sulfide by sulfite reductase (Met5p
and Met10p). Extracellular sulfite can also be reduced to sulfide. Sulfide is sequestered by
O-acetyl-L-homoserine to form methionine and also by serine to form cysteine. Relative to
the rate of sulfide formation, a shortage of precursor compounds (O-acetyl-L-homoserine and
serine) or cofactors (pantothenate or acetyl-CoA) can lead to surplus H 2 S. Under stress condi-
tions caused by nutrient starvation, glutathione can be used as a source of nitrogen with infor-
mation of H 2 S. Methionine can be deaminated and reductively decarboxylated to methionol.
Methanethiol can be formed from methionine by demethiolase and esterified to methanethioac-
etate. Sulfide can also react with ethanol/acetaldehyde to form ethanethiol, and esterified to
ethanethioacetate


can lead to abundant H 2 S production because its uptake is essentially unregulated.


H 2 S is sequestered by the organic nitrogen precursor,O-acetyl-L-homoserine, to


form homocysteine. This latter compound is condensed with serine to produce cys-


teine, which can be incorporated into the sulfur reserve and antioxidant compound


glutathione. Homocysteine is also converted to methionine from which Met-tRNA


andS-adenosylmethionine are produced. Together with cysteine these compounds


regulate the sulfate assimilation pathway.


Degradation of the sulfur amino acids cysteine and methionine to H 2 S and other


volatile sulfur compounds has been observed under laboratory conditions but their


roles under wine fermentation conditions are less clear (Eschenbruch 1974; Jiranek


et al. 1995a; Moreira et al. 2002; Perp`ete et al. 2006; Rankine 1963; Vos and

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