- Gordon, Wei E;
- Baek, Seungbyn;
- Nguyen, Hai P;
- Kuo, Yien-Ming;
- Bradley, Rachael;
- Fong, Sarah L;
- Kim, Nayeon;
- Galazyuk, Alex;
- Lee, Insuk;
- Ingala, Melissa R;
- Simmons, Nancy B;
- Schountz, Tony;
- Cooper, Lisa Noelle;
- Georgakopoulos-Soares, Ilias;
- Hemberg, Martin;
- Ahituv, Nadav
Frugivory evolved multiple times in mammals, including bats. However, the cellular and molecular components driving it remain largely unknown. Here, we use integrative single-cell sequencing (scRNA-seq and scATAC-seq) on insectivorous (Eptesicus fuscus; big brown bat) and frugivorous (Artibeus jamaicensis; Jamaican fruit bat) bat kidneys and pancreases and identify key cell population, gene expression and regulatory differences associated with the Jamaican fruit bat that also relate to human disease, particularly diabetes. We find a decrease in loop of Henle and an increase in collecting duct cells, and differentially active genes and regulatory elements involved in fluid and electrolyte balance in the Jamaican fruit bat kidney. The Jamaican fruit bat pancreas shows an increase in endocrine and a decrease in exocrine cells, and differences in genes and regulatory elements involved in insulin regulation. We also find that these frugivorous bats share several molecular characteristics with human diabetes. Combined, our work provides insights from a frugivorous mammal that could be leveraged for therapeutic purposes.