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      Lantana camara L. (Verbenaceae)

      Fitoterapia
      Elsevier BV

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          Anti-inflammatory actions of pentacyclic triterpenes.

          Pentacyclic triterpenes (PTs) as aglycones of saponins have a wide distribution in plants, and many of them have been used as anti-inflammatory remedies in folk medicine. This survey critically reviews the effects of PTs on proinflammatory mediator signalling pathways and data from experimental animal models and clinical trials. Because the knowledge of their actions is far from being satisfactory a critical summary of the partly promising but mostly scattered and preliminary data might promote productive research on chances and risks of PTs. Antiproliferative and anti-infectious actions and effects on intracellular cell signalling and hormone metabolism are beyond the scope of this short review, although such effects might also contribute to the understanding of the systemic anti-inflammatory actions of aglycones.
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            Biological and pharmacological activity of naturally occurring iridoids and secoiridoids.

            The biological and pharmacological activities reported for naturally occurring iridoids and secoiridoids are reviewed. The hypothesis that iridoid glycoside and acetal esters can best be considered as pro-drugs and that corresponding hemiacetals and compounds derived from them carry the pharmacophores is discussed. The possibility that the activity of some iridoids is determined by their conversion to pyridine monoterpene alkaloids (PMTA) is also considered. The evidence available suggests that iridoids show activities consistent with those presented by immunomodulators and adaptogens.
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              Effects of oleanolic acid and ursolic acid on inhibiting tumor growth and enhancing the recovery of hematopoietic system postirradiation in mice.

              Two triterpene acids, oleanolic acid (OA) and ursolic acid (UA) were examined for their ability to inhibit the tumor growth and modify hematopoiesis after irradiation in three experimental systems: (a) in vivo anti-tumor activity of implanted tumor by ascitic cells was found to be augmented by addition of OA and UA at a high concentration and inhibited in a dose-dependent manner; (b) in the sublethal whole-body irradiated mice treated with the drugs in the 30 min preirradiation period, enhanced effects of OA and UA on peripheral leukocytes were observed by a different significance, and (c) when these chemicals were administered i.p. to mice 30 min before 4 Gy irradiation, both OA and UA enhanced the postirradiation responses of splenic blastogenesis by PHA. UA was a more potent tumorigenic inhibitor than OA. Combining with the gamma-irradiation, however, there was no significant synergetic effect on their anti-tumor activity. The beneficial effects of OA and UA on hematopoiesis and immunocompetence under this study, suggested they might partially play a role in anti-cancer and, furthermore, with the ability to decrease undesirable radiation damage to the hematopoietic tissue after radiotherapy.
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                Journal
                10.1016/S0367-326X(00)00202-1
                http://www.elsevier.com/tdm/userlicense/1.0/

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