The major symptom of Alzheimer's disease (AD) pathology is the accumulation of β-amyloid (Aβ) in the AD patients’ brain; Aβ aggregation may lead to neuronal cell death. Caenorhabditis elegans is a convenient animal model to express organismal complexity. Thus, the purposes of this study is to use human Aβ gene tranginic C. elegans CL4176 and CL2120 to evaluate the effect of leaf extract and four soluble fractions from Rhaphiolepis umbellata var. integerrima on paralyze rate, carbonylated proteins content and Aβ expression in transgenic C. elegans. Results showed that the ethanolic extract and n-hexane soluble fraction reduced Aβ –induced paralysis in transgenic C. elegans CL4176, and its activity was much better than that of positive control, caffeine. It proved that the ethanolic extract and n-hexane soluble fraction from R. umbellata var. integerrima could inhibit Aβ toxicity in C. elegans. The analysis of carbonylated proteins showed that ethyl acetate soluble fraction, n-butanol soluble fraction, and higher concentration of n-hexane soluble fraction reduced carbonylated proteins in C. elegans CL4176 and CL2120. The analysis of Aβ deposits in transgenic C. elegans CL2120 revealed that n-hexane soluble fraction reduced Aβ deposits with the increasing concentration. Effect of n-hexane soluble fraction on decreasing Aβ monomers and Aβ oligomers in C. elegans CL4176 and CL2120 was superior than that of positive control, epigallocatechin-3-gallate (EGCG). According to these results, n-hxexane soluble fraction from R. umbellata var. integerrima could reduce Aβ expression and inhibit Aβ toxicity in transgenic C. elegans.