The relationship between the accumulation of Chl and the apoproteinsof the light-harvesting Chl
a/b-protein complex of PS II (LHCII)during the greening of cucumber cotyledons was studied. LHCIIapoproteins were not detected in etiolated cotyledons. Uponillumination, Chl
a was formed as a result of photoconversionof protochlorophyllide (Pchlide) which had accumulated in thedark. During the lag period that preceded the accumulation ofChl, a small amount of LHCII apoproteins appeared. The amountof LHCII apoproteins increased with increases in levels of Chl
b, though somewhat more rapidly during the first 10 h of greening.Treatment with benzyladenine (BA) or levulinic acid (LA) wasused to vary the supply of Chl
a for apoproteins by promotingor inhibiting the synthesis of Chl
a, respectively. LA decreasedbut BA increased the rate of accumulation of Chl
b and LHCIIapoproteins. Only small amounts of Chl
b and LHCII apoproteinswere formed under intermittent illumination. However, in thepresence of chloramphenicol (CAP), which inhibits the synthesisof plastome-coded proteins including apoproteins of the P700-Chl
a-protein complex (CP1) and a Chl
a-protein complex of PS II(CPa), we observed the accumulation of Chl
b and LHCII apoproteins,both of which are of nuclear origin. During incubation in thedark after intermittent exposure to light, CAP alone allowedneither destruction nor accumulation of Chl
b and LHCII apoproteins,but it did enhance the effect of CaCl
2 in inducing both Chl
b and these apoproteins. These results can be explained by assumingthat apoproteins of CP1 and CPa have a higher affinity for Chl
a than do LHCII apoproteins. When the availability of Chl
ais limited, these apoproteins compete with one another for Chl
a, with the resultant preferential formation of CP1 and CPa.However, when the supply of Chl
a becomes large enough for saturationof apoproteins of CP1 and CPa, some of the Chl
a is incorporatedinto LHCII apoproteins either directly or after conversion toChl
b. Thus, the formation of different Chl-protein complexes(CPs) is regulated by the relative rates of synthesis of Chl
a and apoproteins and by differential affinities of the apoproteinsfor Chl
a.
4Present address: Kyowa Hakko Co., Ltd., 4041, Ami-machi, Inashiki,Ibaraki, 300-03 Japan (Received September 14, 1989; Accepted April 26, 1990)
相似文献