PCP Gene Family in Symbiodinium from Hippopus hippopus: Low Levels of Concerted Evolution, Isoform Diversity, and Spectral Tuning of Chromophores

doi:10.1093/molbev/msg233

MBE Advance Access originally published online on August 29, 2003

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Mol. Biol. Evol. 20(12):2143-2154. 2003
DOI: 10.1093/molbev/msg233
© 2003 by the Society for Molecular Biology and Evolution. ISSN: 0737-4038

PCP Gene Family in Symbiodinium from Hippopus hippopus: Low Levels of Concerted Evolution, Isoform Diversity, and Spectral Tuning of Chromophores

Jay R. Reichman^*^,, Thomas P. Wilcox^* and Peter D. Vize

^* School of Biological Sciences, University of Texas at Austin
Department of Biological Science, University of Calgary, Calgary, Canada

E-mail: reichman.jay{at}epamail.epa.gov.

Photosynthetic dinoflagellates have evolved unique water-solublelight harvesting complexes known as peridinin-chlorophyll a–bindingproteins (PCPs). Most species of dinoflagellates express either14 to 17 kDa or 32 to 35 kDa mature PCP apoproteins and do soin stable combinations of isoforms that differ in isoelectricpoint (pI). The source (posttranslational modification, proteindegradation, or genetic) and functional significance of PCPisoform variation have remained unclear. PCPs are encoded bymultigene families. However, previous reports conflict overthe diversity of PCP genes within gene arrays. We present thefirst genomic characterization of the PCP gene family from asymbiotic dinoflagellate. Symbiodinium from the Pacific bivalveHippopus hippopus (203) contains genes for 33 kDa PCP apoproteinsthat are organized in tandem arrays like those of free-livingdinoflagellates Amphidinium carterae, Lingulodinium (Gonyaulax)polyedra, and Heterocapsa pygmaea. The Symbiodinium 203 PCPcassette consists of 1,098-bp coding regions separated by approximately900-bp spacers. The spacers contain a conserved upstream sequencesimilar to the promoter in L. polyedra. Surprisingly, sequencesof cloned coding regions are not identical, and can differ atup to 2.2% of the nucleotide sites. Sequence variation is foundat both silent and nonsilent sites, and analysis of cDNA clonesindicate that the variation is present in the mRNA pool. Wepropose that this variation represents nucleotide diversityamong PCP gene copies that are evolving under low-level concertedevolution. Interestingly, the predicted proteins have pIs thatare within the range of those published for other species ofSymbiodinium. Thus, posttranslational modifications are notnecessary to explain the multiple PCP isoforms. We have alsoidentified several polymorphic sites that may influence spectralabsorption tuning of chromophores.

Key Words: peridinin • PCP • gene family • dinoflagellate • Symbiodinium • concerted evolution

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