A reference genome for the long-term kleptoplast-retaining sea slugElysia crispatamorphotype clarki

Author:

Eastman Katharine E12ORCID,Pendleton Amanda L12ORCID,Shaikh Mearaj A23ORCID,Suttiyut Thiti23ORCID,Ogas Raeya12,Tomko Paxton24ORCID,Gavelis Gregory12ORCID,Widhalm Joshua R23ORCID,Wisecaver Jennifer H12ORCID

Affiliation:

1. Department of Biochemistry, Purdue University , West Lafayette, IN 47907 , USA

2. Purdue Center for Plant Biology, Purdue University , West Lafayette, IN 47907 , USA

3. Department of Horticulture and Landscape Architecture, Purdue University , West Lafayette, IN 47907 , USA

4. Department of Biological Sciences, Purdue University , West Lafayette, IN 47907 , USA

Abstract

AbstractSeveral species of sacoglossan sea slugs possess the incredible ability to sequester chloroplasts from the algae they consume. These “photosynthetic animals” incorporate stolen chloroplasts, called kleptoplasts, into the epithelial cells of tubules that extend from their digestive tracts throughout their bodies. The mechanism by which these slugs maintain functioning kleptoplasts in the absence of an algal nuclear genome is unknown. Here, we report a draft genome of the sacoglossan slug Elysia crispata morphotype clarki, a morphotype native to the Florida Keys that can retain photosynthetically active kleptoplasts for several months without feeding. We used a combination of Oxford Nanopore Technologies long reads and Illumina short reads to produce a 786-Mb assembly (N50 = 0.459 Mb) containing 68,514 predicted protein-coding genes. A phylogenetic analysis found no evidence of horizontal acquisition of genes from algae. We performed gene family and gene expression analyses to identify E. crispata genes unique to kleptoplast-containing slugs that were more highly expressed in fed versus unfed developmental life stages. Consistent with analyses in other kleptoplastic slugs, our investigation suggests that genes encoding lectin carbohydrate-binding proteins and those involved in regulation of reactive oxygen species and immunity may play a role in kleptoplast retention. Lastly, we identified four polyketide synthase genes that could potentially encode proteins producing UV- and oxidation-blocking compounds in slug cell membranes. The genome of E. crispata is a quality resource that provides potential targets for functional analyses and enables further investigation into the evolution and mechanisms of kleptoplasty in animals.

Funder

Purdue University

Publisher

Oxford University Press (OUP)

Subject

Genetics (clinical),Genetics,Molecular Biology

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