This study aimed to investigate the active ingredients of the MeOH extract of Mondia whitei L., which belongs to Asclepiadaceae. Preliminary results indicated that its hexane and water layer possess anti-hyperglycemic activity and ethyl acetate layer possess anti-angiogenesis activity. Thirty four compounds were isolated via various chromatographic techniques and their structures were further identified according to their physical data, NMR. They are 2-Hydroxy-4-methoxybenzaldehyde (1), L-Phenylalanine (2), Oleanolic acid acetate (3), Oleanolic acid (4), Oleanolic aldehyde acetate (5), Lantanone (6), β-Amyrin acetate (7), α-Amyrin acetate (8), β-Sitosterone (9), 6β-Hydroxystigmast-4-en-3-one (10), 6β-Hydroxystigmasta-4, 22 -dien-3-one (11), mixture of β-Sitosterol (12) and Stigmasterol (13), β-Sitosterol-3-O-β-D-glucoside (14), Palmitic acid (15), Stearic acid (16), mixture of Linoleic acid (17) and Linolenic acid (18), mixture of Methyl palmitate (19) and Methyl linoleate (20), Uridine (21), Adenosine (22), Myo-inositol (23), Tyrosol (24), Methyl caffeate (25), Methyl chlorogenate (26), Osthole (27), Bergenin (28), (+)-Lariciresinol (29), (+)-Catechin (30), Quercetin (31)、Rutin (32), Isoquecetrin (33), and Hyperoside (34). According to their skeletons, those identified compounds can be classified into Amino acid: 2, Triterpenoids: 3∼8, Steroids: 9∼14, Fatty acid: 15∼20, Nucleosides: 21~22, C6 Sugar alcohol: 23, Phenolics: 1, 24~26, Coumarins: 27, Isocoumarin: 28, Lignans: 29, Flavonoids: 30~34. Among the isolates from the hexane layer , 1 μM of the compounds 3, 4 , 6 , 7 , 8 were demonstrated to enhance glucose uptake to 117.66 ± 2.41%, 109.47 ± 2.83%, 124.56 ± 3.31%, 108.71 ± 0.85%, 108.38 ± 2.02%, respectively, using a mouse myoblast cell (C2C12) culture system. Among the isolates from the ethyl acetate layer, 30 μM of the compounds 25 and 31 inhibited 32.95 ± 2.51%, 80.67± 3.43 % HUVEC cell proliferations.