Cooperation of LPA3 and LPA2 Is Essential for Photosystem II Assembly in Arabidopsis

Photosystem II (PSII) is a multisubunit membrane protein complex that is assembled in a sequence of steps. However, the molecular mechanisms responsible for the assembly of the individual subunits into functional PSII complexes are still largely unknown. Here, we report the identification of a chloroplast protein, Low PSII Accumulation3 (LPA3), which is required for the assembly of the CP43 subunit in PSII complexes in Arabidopsis (Arabidopsis thaliana). LPA3 interacts with LPA2, a previously identified PSII CP43 assembly factor, and a double mutation of LPA2 and LPA3 is more deleterious for assembly than either single mutation, resulting in a seedling-lethal phenotype. Our results indicate that LPA3 and LPA2 have overlapping functions in assisting CP43 assembly and that cooperation between LPA2 and LPA3 is essential for PSII assembly. In addition, we provide evidence that LPA2 and LPA3 interact with Albino3 (Alb3), which is essential for thylakoid protein biogenesis. Thus, the function of Alb3 in some PSII assembly processes is probably mediated through interactions with LPA2 and LPA3.Oxygenic photosynthesis, in which oxygen and organic carbon are produced from water and carbon dioxide using sunlight, provides energy for nearly all living organisms on Earth. Four major multiprotein complexes, located in thylakoid membranes, are responsible for the capture of light and its conversion to chemical energy in eukaryotic photosynthetic organisms: PSI, PSII, cytochrome b₆/f, and ATP synthase (Wollman et al., 1999; Nelson and Yocum, 2006). PSII catalyzes one of the most important of all biochemical reactions, the light-induced transfer of electrons from water to plastoquinone, which generates most of the oxygen in the Earth’s atmosphere. PSII consists of more than 20 subunits in higher plants (Wollman et al., 1999; Iwata and Barber, 2004; Nelson and Yocum, 2006). The PSII reaction center consists of the D1 and D2 proteins, the α- and β-subunits of cytochrome b₅₅₉, and the PsbI protein, and the D1 and D2 heterodimers bind all the redox components essential for the primary charge separation (Nanba and Satoh, 1987). The PSII core complex additionally contains CP47, CP43, the oxygen-evolving complex, and several low molecular mass proteins (Wollman et al., 1999; Nelson and Yocum, 2006). CP47 and CP43, two inner chlorophyll a-binding proteins, are closely associated with, and located on opposite sides of, the PSII reaction center (Hankamer et al., 1999). The functional form of PSII cores in thylakoid membranes is dimeric and is associated with light-harvesting complex (LHC). In PSII-LHCII supercomplexes, PSII core dimers are surrounded by LHCII trimers, which consist of Lhcb1 and Lhcb2 proteins (Wollman et al., 1999; Iwata and Barber, 2004; Nelson and Yocum, 2006).Our knowledge of the molecular mechanisms involved in the biogenesis and assembly of PSII in the thylakoid membranes is still limited, although the structure and function of PSII have been extensively studied. Genetic and biochemical studies have elucidated several distinct steps that occur in PSII assembly. D2 and cytochrome b₅₅₉ form an initial complex, which serves as a receptor for the cotranslational assembly of D1 (Adir et al., 1990; van Wijk et al., 1997; Müller and Eichacker, 1999; Zhang et al., 1999). The next step involves the association of CP47 with the PSII reaction center (Zhang et al., 1999; Rokka et al., 2005), while CP43 is synthesized independently and then continuously associates and dissociates with PSII (de Vitry et al., 1989; Zhang et al., 2000). The biogenesis of PSII involves “a control by epistasy of synthesis” process (Minai et al., 2006). D2 is required for D1 synthesis, which itself is needed for CP47 synthesis. However, many aspects of the processes involved in the oligomerization and coordination of the various PSII subunits are still unclear (Rochaix, 2001). Due to the structural complexity of PSII, its assembly consists of multiple assembly steps, which is likely to require the participation of a number of assembly factors.Several assembly factors involved in the biosynthesis and assembly of the PSII complex have been identified recently. For instance, the thylakoid lumen protein HCF136 is known to be required for the formation of PSII, since the hcf136 mutant is capable of synthesizing plastid-encoded proteins, but it does not appear to accumulate any stable PSII complexes, due to blockage of the assembly of the PSII reaction center (Meurer et al., 1998; Plücken et al., 2002). Alb3.1, a homolog of Arabidopsis (Arabidopsis thaliana) Albino3 (Alb3), is essential for the efficient assembly of PSII in Chlamydomonas reinhardtii, probably through interactions with D1 following its insertion (Ossenbühl et al., 2004), and another Alb3 homolog, Alb3.2, appears to be required for photosystem assembly in Chlamydomonas (Göhre et al., 2006). Coimmunoprecipitation analysis has shown that Alb3.1 and Alb3.2 interact directly, while Alb3.2 reportedly interacts with the PSI and PSII reaction centers proteins (Göhre et al., 2006). The lumenal immunophilins, AtCYP38 and FKBP20-2, have also been shown to be involved in PSII assembly (Lima et al., 2006; Fu et al., 2007; Sirpiö et al., 2008). In addition, we recently identified two PSII assembly factors, Low PSII Accumulation1 (LPA1) and LPA2, involved in PSII assembly. The LPA1 protein appears to be an integral membrane chaperone required for efficient assembly of the PSII core complex, probably through direct interaction with D1 (Peng et al., 2006). LPA2, which interacts with Alb3, forms a protein complex that assists CP43 assembly within PSII (Ma et al., 2007). These findings suggest that each stage of the PSII assembly process is assisted by one or more specific assembly factors, most of which have not yet been identified.Here, we report the identification of a lpa3 mutant with reduced levels of PSII. Functional characterization points to the possible role of LPA3 in assisting CP43 assembly within PSII. In addition, biochemical and genetic analyses indicate that an assembly complex of LPA3 and LPA2 is essential for PSII assembly.