Various extracts of the marine brown alga Endarachne binghamiae were assayed in vitro for inhibiting the proliferation in human breast adenocarcinoma cell （MDA-MB-231）, human hepatoblastoma cell（Hep G2）and human pancreatic cell （MIA PaCa-2）. In the present study, fucoidan, alginic acid, calcium alginate and sodium alginate extracted from the brown alga Petalonia binghamiae inhibited markedly the proliferation in carcinoma cells. The inhibitory reaction of sodium alginate decreased after being treated with citrate buffer solution and lost in the presence of Ca2+, Zn2+, Co2+ or Mn2+. However, sodium alginate remained high inhibitory activity if metal ions were treated with Na2EDTA prior to addition to culture medium. These results showed that ion exchange at carboxyl groups as well as molecule conformation of the polymer played an important role in alginate inhibitory reaction with carcinoma cells. Moreover, the obtained sodium alginate induced murine macrophages to produce proteinaeous substance that significantly inhibited carcinoma cell proliferation. My study suggests that sodium alginate has using potential in anticancer therapy and research due to its wide distribution and high production in marine brown algae. A novel protein assigned as EBP (Endarachne binghamiae protein) was obtained after being extracted in phosphate buffered saline, precipitated by saturated ammonium sulfate and finally purified by gel filtration and ion-exchange column chromatography. The purified protein has molecular weight of 69 kDa. It is a monomer glycoprotein, containing 20.37 % carbohydrate moiety. The EBP is rather stable in immunity while subjected to 121℃ and a wide range of pH values (3.0~12.0). The above findings suggests that the reported alga is a promising source of proteins and polysaccharides. In detail research, we are looking forward to seeing that immunostimulation and immuno-modulation can be used as medicine in cancer therapy.