Carrier-Mediated Uptake and Phloem Systemy of a 350-Dalton Chlorinated Xenobiotic with an α-Amino Acid Function1
In a previous paper we have shown that ε-(phenoxyalkanecarboxylyl)- l -Lys conjugates are potent inhibitors of amino acid transport systems and that it is possible to modulate the uptake inhibition by hydrophobic or hydrophilic additions in the 4-position of the aromatic ring (J.F. Chollet, C. Delét...
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Veröffentlicht in: | Plant physiology (Bethesda) 2001-04, Vol.125 (4), p.1620-1632 |
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Sprache: | eng |
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Zusammenfassung: | In a previous paper we have shown that
ε-(phenoxyalkanecarboxylyl)-
l
-Lys conjugates are potent
inhibitors of amino acid transport systems and that it is possible to
modulate the uptake inhibition by hydrophobic or hydrophilic additions
in the 4-position of the aromatic ring (J.F. Chollet, C.
Delétage, M. Faucher, L. Miginiac, J.L. Bonnemain [1997]
Biochem Biophys Acta 1336: 331–341). In this report we
demonstrate that ε-(2,4-dichlorophenoxyacetyl)-
l
-Lys
(2,4D-Lys), one of the largest molecules of the series and one of the
most potent inhibitors, is a highly permeant conjugate. Uptake of
2,4D-Lys by broad bean (
Vicia faba
) leaf discs is
mediated by an active carrier system
(
K
m
1 = 0.2 m
m
;
V
max
1 = 2.4 nmol cm
−2
h
−1
at pH 5.0) complemented by an important diffusive
component. Among the compounds tested (neutral, basic, and acidic amino
acids, auxin, glutathione, and sugars), only the aromatic amino acids
clearly compete with 2,4D-Lys. The conjugate accumulates in the vein
network, is exported toward the growing organs, and exhibits a
distribution pattern different from that of the herbicide moiety.
However, over time 2,4D-Lys progressively splits into 2,4D and lysine.
Analyses by high-performance liquid chromatography and liquid
scintillation spectrometry of the phloem sap collected from the castor
bean system, used as a systemy test, indicate decreasing
capacities of 2,4D, 2,4D-Lys, and glyphosate, respectively, to move
from the epidermis cell wall to the sieve element. Our results show
that it is possible to design synthesis of large-size xenobiotics
(approximately 350 D) with a lipophilic pole, exhibiting high mobility
within the vascular system. |
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ISSN: | 0032-0889 1532-2548 |