Antitumor activity of extracts from Peperomia elongata

Abstract The cytotoxic potential of ethanol extracts from Peperomia elongata. H. B. & K. (Piperaceae) were evaluated against human cancer cell lines by the MTT method. The samples considered cytotoxic were tested for antimitotic activity with the sea urchin egg development test and for hemolytic...

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Veröffentlicht in:	Pharmaceutical biology 2007-01, Vol.45 (10), p.760-765
Hauptverfasser:	Campos, P.B. de C, Gama, J.J.T, Pereira, L.P, Costa-Lotufo, L.V, Moraes, M.O. de, Guimaraes, E.F, Kato, M.J, Furlan, M, Pessoa, C
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Sprache:	eng
Schlagworte:	anticarcinogenic activity antimitotic activity antineoplastic agents Antitumor cytotoxic activity cytotoxicity cytotoxins leaves Lytechinus variegatus medicinal plants MTT assay Peperomia Piperaceae plant extracts roots stems
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container_title	Pharmaceutical biology
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creator	Campos, P.B. de C Gama, J.J.T Pereira, L.P Costa-Lotufo, L.V Moraes, M.O. de Guimaraes, E.F Kato, M.J Furlan, M Pessoa, C
description	Abstract The cytotoxic potential of ethanol extracts from Peperomia elongata. H. B. & K. (Piperaceae) were evaluated against human cancer cell lines by the MTT method. The samples considered cytotoxic were tested for antimitotic activity with the sea urchin egg development test and for hemolytic activity using mice erythrocytes. The extracts from leaves (hexane), stems (ethanol, hexane, hexane:AcOEt, AcOEt, and MeOH:H2O insoluble), and roots (R4) presented potential cytotoxic action. The stems extracts showed the highest toxicity in all tumor cell lines tested, with an IC50 ≤ 9.0 µg mL for ethanol extract, IC50 ≤ 11.6 µg mL for MeOH:H2O insoluble, IC50 ≤ 7.3 µg mL for hexane extract, IC50 ≤ 11.4 µg mL for hexane: AcOEt, and IC50 ≤ 16.2 µg mL for AcOEt extract. All extracts considered cytotoxic for tumoral cell lines presented antimitotic activity. The samples from roots (R4) and stems (ethanol, MeOH:H2O insoluble, and hexane extract from leaves) were found to possess lytic activity in mice erythrocytes but in higher doses (> 125 µg mL). Further studies for the isolation and identification of the active principles of these extracts should be undertaken.
doi_str_mv	10.1080/13880200701585857
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H. B. & K. (Piperaceae) were evaluated against human cancer cell lines by the MTT method. The samples considered cytotoxic were tested for antimitotic activity with the sea urchin egg development test and for hemolytic activity using mice erythrocytes. The extracts from leaves (hexane), stems (ethanol, hexane, hexane:AcOEt, AcOEt, and MeOH:H2O insoluble), and roots (R4) presented potential cytotoxic action. The stems extracts showed the highest toxicity in all tumor cell lines tested, with an IC50 ≤ 9.0 µg mL for ethanol extract, IC50 ≤ 11.6 µg mL for MeOH:H2O insoluble, IC50 ≤ 7.3 µg mL for hexane extract, IC50 ≤ 11.4 µg mL for hexane: AcOEt, and IC50 ≤ 16.2 µg mL for AcOEt extract. All extracts considered cytotoxic for tumoral cell lines presented antimitotic activity. The samples from roots (R4) and stems (ethanol, MeOH:H2O insoluble, and hexane extract from leaves) were found to possess lytic activity in mice erythrocytes but in higher doses (> 125 µg mL). 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H. B. & K. (Piperaceae) were evaluated against human cancer cell lines by the MTT method. The samples considered cytotoxic were tested for antimitotic activity with the sea urchin egg development test and for hemolytic activity using mice erythrocytes. The extracts from leaves (hexane), stems (ethanol, hexane, hexane:AcOEt, AcOEt, and MeOH:H2O insoluble), and roots (R4) presented potential cytotoxic action. The stems extracts showed the highest toxicity in all tumor cell lines tested, with an IC50 ≤ 9.0 µg mL for ethanol extract, IC50 ≤ 11.6 µg mL for MeOH:H2O insoluble, IC50 ≤ 7.3 µg mL for hexane extract, IC50 ≤ 11.4 µg mL for hexane: AcOEt, and IC50 ≤ 16.2 µg mL for AcOEt extract. All extracts considered cytotoxic for tumoral cell lines presented antimitotic activity. The samples from roots (R4) and stems (ethanol, MeOH:H2O insoluble, and hexane extract from leaves) were found to possess lytic activity in mice erythrocytes but in higher doses (> 125 µg mL). Further studies for the isolation and identification of the active principles of these extracts should be undertaken.</description><subject>anticarcinogenic activity</subject><subject>antimitotic activity</subject><subject>antineoplastic agents</subject><subject>Antitumor</subject><subject>cytotoxic activity</subject><subject>cytotoxicity</subject><subject>cytotoxins</subject><subject>leaves</subject><subject>Lytechinus variegatus</subject><subject>medicinal plants</subject><subject>MTT assay</subject><subject>Peperomia</subject><subject>Piperaceae</subject><subject>plant extracts</subject><subject>roots</subject><subject>stems</subject><issn>1388-0209</issn><issn>1744-5116</issn><fulltext>true</fulltext><rsrctype>article</rsrctype><creationdate>2007</creationdate><recordtype>article</recordtype><recordid>eNp9j91Kw0AQhRdRsFYfwCvzAtHZv2yC3pTiHxQUtNfLJNltU5Js2WzVvL0r9UaEMhdnhplvDoeQSwrXFHK4oTzPgQEooDKPpY7IhCohUklpdhz7uE_jQXFKzoZhAwCSczkh2awPTdh1zidYheajCWPibGK-go_zkFjvuuTVbE3UBhPTun6FAc_JicV2MBe_OiXLh_v3-VO6eHl8ns8WacVZFlJpstIwCZVSeV1KmpVSFFzYEozJy9pShZzWmeAARUmtKBivsFSqYIwyLmo-JXT_t_JuGLyxeuubDv2oKeif4Ppf8Mjc7Zmmt853-Ol8W-uAY-u89dhXzaD5Ifz2D7422IZ1hd7ojdv5PsY9aH61py06jSsfvZZvDGhMmItMSsa_AVMxePo</recordid><startdate>20070101</startdate><enddate>20070101</enddate><creator>Campos, P.B. de C</creator><creator>Gama, J.J.T</creator><creator>Pereira, L.P</creator><creator>Costa-Lotufo, L.V</creator><creator>Moraes, M.O. de</creator><creator>Guimaraes, E.F</creator><creator>Kato, M.J</creator><creator>Furlan, M</creator><creator>Pessoa, C</creator><general>Informa UK Ltd</general><general>Taylor & Francis</general><scope>FBQ</scope><scope>AAYXX</scope><scope>CITATION</scope></search><sort><creationdate>20070101</creationdate><title>Antitumor activity of extracts from Peperomia elongata</title><author>Campos, P.B. de C ; Gama, J.J.T ; Pereira, L.P ; Costa-Lotufo, L.V ; Moraes, M.O. de ; Guimaraes, E.F ; Kato, M.J ; Furlan, M ; Pessoa, C</author></sort><facets><frbrtype>5</frbrtype><frbrgroupid>cdi_FETCH-LOGICAL-c326t-5e6be250c778db516b54934fb0ee8bdf17a31d643009b1f4923cab779221234d3</frbrgroupid><rsrctype>articles</rsrctype><prefilter>articles</prefilter><language>eng</language><creationdate>2007</creationdate><topic>anticarcinogenic activity</topic><topic>antimitotic activity</topic><topic>antineoplastic agents</topic><topic>Antitumor</topic><topic>cytotoxic activity</topic><topic>cytotoxicity</topic><topic>cytotoxins</topic><topic>leaves</topic><topic>Lytechinus variegatus</topic><topic>medicinal plants</topic><topic>MTT assay</topic><topic>Peperomia</topic><topic>Piperaceae</topic><topic>plant extracts</topic><topic>roots</topic><topic>stems</topic><toplevel>peer_reviewed</toplevel><toplevel>online_resources</toplevel><creatorcontrib>Campos, P.B. de C</creatorcontrib><creatorcontrib>Gama, J.J.T</creatorcontrib><creatorcontrib>Pereira, L.P</creatorcontrib><creatorcontrib>Costa-Lotufo, L.V</creatorcontrib><creatorcontrib>Moraes, M.O. de</creatorcontrib><creatorcontrib>Guimaraes, E.F</creatorcontrib><creatorcontrib>Kato, M.J</creatorcontrib><creatorcontrib>Furlan, M</creatorcontrib><creatorcontrib>Pessoa, C</creatorcontrib><collection>AGRIS</collection><collection>CrossRef</collection><jtitle>Pharmaceutical biology</jtitle></facets><delivery><delcategory>Remote Search Resource</delcategory><fulltext>fulltext</fulltext></delivery><addata><au>Campos, P.B. de C</au><au>Gama, J.J.T</au><au>Pereira, L.P</au><au>Costa-Lotufo, L.V</au><au>Moraes, M.O. de</au><au>Guimaraes, E.F</au><au>Kato, M.J</au><au>Furlan, M</au><au>Pessoa, C</au><format>journal</format><genre>article</genre><ristype>JOUR</ristype><atitle>Antitumor activity of extracts from Peperomia elongata</atitle><jtitle>Pharmaceutical biology</jtitle><date>2007-01-01</date><risdate>2007</risdate><volume>45</volume><issue>10</issue><spage>760</spage><epage>765</epage><pages>760-765</pages><issn>1388-0209</issn><eissn>1744-5116</eissn><abstract>Abstract The cytotoxic potential of ethanol extracts from Peperomia elongata. H. B. & K. (Piperaceae) were evaluated against human cancer cell lines by the MTT method. The samples considered cytotoxic were tested for antimitotic activity with the sea urchin egg development test and for hemolytic activity using mice erythrocytes. The extracts from leaves (hexane), stems (ethanol, hexane, hexane:AcOEt, AcOEt, and MeOH:H2O insoluble), and roots (R4) presented potential cytotoxic action. The stems extracts showed the highest toxicity in all tumor cell lines tested, with an IC50 ≤ 9.0 µg mL for ethanol extract, IC50 ≤ 11.6 µg mL for MeOH:H2O insoluble, IC50 ≤ 7.3 µg mL for hexane extract, IC50 ≤ 11.4 µg mL for hexane: AcOEt, and IC50 ≤ 16.2 µg mL for AcOEt extract. All extracts considered cytotoxic for tumoral cell lines presented antimitotic activity. The samples from roots (R4) and stems (ethanol, MeOH:H2O insoluble, and hexane extract from leaves) were found to possess lytic activity in mice erythrocytes but in higher doses (> 125 µg mL). Further studies for the isolation and identification of the active principles of these extracts should be undertaken.</abstract><pub>Informa UK Ltd</pub><doi>10.1080/13880200701585857</doi><tpages>6</tpages></addata></record>
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subjects	anticarcinogenic activity antimitotic activity antineoplastic agents Antitumor cytotoxic activity cytotoxicity cytotoxins leaves Lytechinus variegatus medicinal plants MTT assay Peperomia Piperaceae plant extracts roots stems
title	Antitumor activity of extracts from Peperomia elongata
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