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177893

ANTITUMOR AND ANTIANGIOGENIC EFFECTS OF THALIDOMIDE, ROFECOXIB, AND CAPTOPRIL IN EHRLICH ASCITES CARCINOMA IN MICE

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Last updated: 22 Jan 2023

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Abstract

The study was conducted to evaluate the effect of thalidomide, rofecoxib and captopril on tumor growth and survival, when used alone or in combinatiun with cisplatin in Swiss albino mice Solid tumors were induced by a subcutaneous injection of Ehrlich ascites carcinoma (EAC) Cells .The antiangiogenic activity of these drugs as studied to explore the potential mechanism involved.
The EAC cells implanted subcutaneously to produce a solid tumor in the right flank of Swiss albino mice .This tumor was used to evaluate the anti-tumor and anti-angiogenic activities of thalidomide (100 mg/kg, i.p.) rofecoxib  (20 mg/kg, p.o. ) or captopril(50 mg kg, p.o.)as individual treatments or in combination with cisplatin (2 mg/kg ,i.p.) All treatment, were started 24 hours after tumor cells inoculation .Tumor size was measured every other day for 21days, tumor growth time (TGT) and tumor growth  delay time (TGDT) were calculated Animals were monitored and the mortality was recorded daily along the study period (100 days) to calculate the percentage survival of animals, mean survival time( MST) and percentage increased life span (%ILS).In a parallel experiment,  the degree of angiogenesis was assessed by measuring the tumor vascular volume spectrophotometrically  using 1% (w/v) Evan's blue.
Individual treatments with thalidomide, rofecoxib or captopril produced a significant(p≤0.001) reduction in tumor volume as Compared to the control group. Their depressing effect on tumor volume tended to be enhanced progressively from the individual  treatment to the combinations with cisplatin .The treatment with cisplatin, thalidomide and their combination could expand the life span of animals for 86,96 and 100 days respectively . Thalidomide and rofecoxib significantly (p≤0.05) inhibited the  angiogenesis  compared to the control group. The combination of cisplatin with thalidomide or rofecoxib further inhibited the angiogenesis significantly compared to the control group (p≤0.001) as well as cisplatin-treated group (p≤0.01). In the contrast, a significant inhibitory effect of captopril or cisplatin on angiogenesis was not evident. However, the combination of captopril and cisplatin could produce a significant inhibition of angiogenesis (p < 0.001).
These data indicate that thalidomide, rofecoxib, or captopril exerts an antitumorigenic effect on EAC solid tumor in Swiss mice. Thalidomide and rofecoxib proved to have an antiangiogenic effect in EAC-model. Our results suggest the use of antiangiogenic agents as an adjuvant treatment to chemotherapy.

DOI

10.21608/zjps.2005.177893

Authors

First Name

El-Sayed

Last Name

El-Awady

MiddleName

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Affiliation

Department of Pharmacology and Toxicology, Faculty of Pharmacy, Suez Canal University. Ismailia, Egypt

Email

el-sayed.el-awady@yahoo.com

City

-

Orcid

-

First Name

Mona

Last Name

EI-Azab

MiddleName

-

Affiliation

Department of Pharmacology, Faculty of Pharmacy, Suez Canal University, Ismailia, Egypt

Email

mona.ei-azab@yahoo.com

City

-

Orcid

-

First Name

Yasser

Last Name

Moustafa

MiddleName

-

Affiliation

Department of Pharmacology, Faculty of Pharmacy, Suez Canal University, Ismailia, Egypt

Email

yasser.moustafa@yahoo.com

City

-

Orcid

-

First Name

Alaa

Last Name

Abd-El-Hameed

MiddleName

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Affiliation

Department of Clinical Pathology, Faculty of Medicine. Suez Canal University, Ismailia, Egypt

Email

alaa.abd-el-hameed@yahoo.com

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-

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Volume

14

Article Issue

1

Related Issue

24750

Issue Date

2005-06-01

Receive Date

2005-04-24

Publish Date

2005-06-01

Page Start

48

Page End

57

Print ISSN

1110-5089

Online ISSN

2356-9786

Link

https://zjps.journals.ekb.eg/article_177893.html

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https://zjps.journals.ekb.eg/service?article_code=177893

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7

Type

Original Article

Type Code

862

Publication Type

Journal

Publication Title

Zagazig Journal of Pharmaceutical Sciences

Publication Link

https://zjps.journals.ekb.eg/

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Article

Created At

22 Jan 2023