| Literature DB >> 22943788 |
Margaret E M Farias1, Carter T Atkinson, Dennis A LaPointe, Susan I Jarvi.
Abstract
BACKGROUND: The avian disease system in Hawaii offers an ideal opportunity to investigate host-pathogen interactions in a natural setting. Previous studies have recognized only a single mitochondrial lineage of avian malaria (Plasmodium relictum) in the Hawaiian Islands, but cloning and sequencing of nuclear genes suggest a higher degree of genetic diversity.Entities:
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Year: 2012 PMID: 22943788 PMCID: PMC3489548 DOI: 10.1186/1475-2875-11-305
Source DB: PubMed Journal: Malar J ISSN: 1475-2875 Impact factor: 2.979
Figure 1Distribution of composite trap genotypes by study site map of eastern Hawaii Island showing locations of 1 sq km study sites (red squares). Solid lines indicate 250 m elevational contours. High-elevation sites are (1) CJ Ralph and (2) Solomon’s, mid-elevation sites are (3) Ainahou Ranch, (4) Crater Rim, (5) Cooper’s, (6) Puu Unit and (7) Waiakea, and low-elevation sites are (8) Bryson’s, (9) Nanawale, and (10) Malama Ki.
Composite genotypes
| 1 | T | A | G | 92 |
| 2 | T | A | C | 11 |
| 3 | T | A | G/C | 13 |
| 4 | T/C | A | G | 3 |
| 5 | T | A/G | G | 2 |
Composite trap genotypes based on standard and modified single base extension reactions for loci 539, 1178 and 1293. The remaining five loci were monomorphic in this study. N, overall number of hatch-year amakihi infected with each composite trap genotype.
Figure 2Predicted probability of infection with genotype 2 or 3. Predicted probability of infection (P) with genotype 2 or 3 based on the best linear regression model plotted as a function of Mosquito Capture Rate (A) over all sites and (B) over low-elevation sites only.