Autotaxin is an extracellular, two zinc-centered enzyme that hydrolyzes lysophosphatidyl choline to lysophosphatidic acid, involved in various cancerous processes, e.g. migration, proliferation and tumor progression. We examined the autotaxin inhibitory properties of extended structure carbamoylphosphonates (CPOs) PhOC 6 H 4 SO 2 NH(CH 2 ) n NHCOPO 3 H 2 , with increasing lengths of methylene chains, (CH 2 ) n , n ¼ 4-8. Carbamoylphosphonates having n ¼ 6, 7, 8 inhibited autotaxin in vitro with IC 50 & 1.5 mM. Using an imaging probe we demonstrated that compound n ¼ 6 inhibits recombinant autotaxin activity in vitro and in vivo, following oral CPO administration. Additionally, daily oral administration of compound n ¼ 7 inhibited over 90% of lung metastases in a murine melanoma metastasis model. Both the carbamoylphosphonates and the enzymes reside and interact in the extracellular space expecting minimal toxic side effects, and presenting a novel approach for inhibiting tumor proliferation and metastasis dissemination.