Angiotensin-Il Receptor Blockers (ARB)

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Drug Name Angiotensin-Il Receptor Blockers (ARB)
FDA Approval Not specified
Used for Not specified
Clinical Trial Phase Not specified
Clinical Trial Explanation Not specified
Common Side Effects Not specified
OS without Not specified
OS with Not specified
PFS without Not specified
PFS with Not specified
Usefulness Rating Not rated
Usefulness Explanation Not specified
Toxicity Level Not specified
Toxicity Explanation Not specified



From Ben Williams Book: Angiotensin-II is a peptide hormone produced from angiotensin-I by the action of angiotensin converting enzyme (ACE). The main effect of angiotensin-II is vasoconstriction and a resulting increase in blood pressure. Therefore ACE inhibitors and angiotensin-II receptor blockers are used as anti-hypertensive drugs, especially in heart disease. More recently these drugs have been repurposed for use in cancer studies.

A retrospective study published in 2012 (328) examined the steroid-sparing effects of angiotensin-II inhibitors, incuding ACE inhibitors and angiotensin-II receptor blockers (ARBs). Of a total cohort of 87 newly diagnosed glioblastoma patients, 29 patients were identified who were treated prior to radiation for high blood pressure. 18 of these were treated with either ACE inhibitors (n=3) or angiotensin-II receptor blockers (n=15). Although no survival benefit with angiotensin-II inhibitors was observed in this study, the 18 patients treated with an angiotensin-II inhibitor required half the steroid dose compared to all other patients in the study (mean prednisolone dose of 29 mg per day versus 60 mg per day), and this difference remained significant in multivariate analysis (p=0.003).

A later retrospective study by the same group published in January 2016 (329) focused specifically on the angiotensin-II receptor blocker class of drugs and their effects on vasogenic edema in glioblastoma patients. In this study, 11 patients taking angiotensin-II receptor blockers (ARBs) for hypertension were compared with 11 matched patients with similar age, tumor size, and tumor location, but not taking medication for hypertension. There was a significant 66% reduction in the FLAIR ratio in the patients taking ARBs compared to the matched patients not taking ARBs. As FLAIR signal can represent either tumor infiltration or vasogenic edema, the nature of the peri-tumoral FLAIR signal was assessed with apparent diffusion coeffient (ADC) mapping. Nine evaluable patients taking 28

ARBs had a 34% reduction in ADC ratios compared to their matched controls not taking ARBs, confirming the ability of this class of drugs to reduce peri-tumoral edema.

A 2015 study, also by the group in France, suggests angiotensin-II inhibitors (including ACE inhibitors and ARBs) may also lead to superior survival outcomes (330). In this study, 81 GBM patients were included. Seven of these patients were taking ACE inhibitors and 19 were taking ARBs for hypertension. The 26 patients using angiotensin-II inhibitors had increased progression-free and overall survival (8.7 and 16.7 months) compared to the patients not taking these drugs (7.2 and 12.9 months). Use of angiotensin-II inhibitors was a significant positive prognostic factor for both PFS and OS in multivariate analysis.

A randomized phase 3 trial in France (NCT01805453) has recently completed recruitment, and is testing the influence of losartan (an ARB) versus placebo on the steroid dose required to control edema on the last day of radiotherapy. Another drug in this class, telmisartan, has superior penetration into the central nervous system (331) and may therefore be a better choice.

See Chapter 13 for a discussion of Angiotensin system inhibitors plus AvastinProperty "Has original text" (as page type) with input value "Angiotensin-II is a peptide hormone produced from angiotensin-I by the action of</br>angiotensin converting enzyme (ACE). The main effect of angiotensin-II is</br>vasoconstriction and a resulting increase in blood pressure. Therefore ACE inhibitors and</br>angiotensin-II receptor blockers are used as anti-hypertensive drugs, especially in heart</br>disease. More recently these drugs have been repurposed for use in cancer studies.</br></br>A retrospective study published in 2012 (328) examined the steroid-sparing effects of</br>angiotensin-II inhibitors, incuding ACE inhibitors and angiotensin-II receptor blockers</br>(ARBs). Of a total cohort of 87 newly diagnosed glioblastoma patients, 29 patients were</br>identified who were treated prior to radiation for high blood pressure. 18 of these were</br>treated with either ACE inhibitors (n=3) or angiotensin-II receptor blockers (n=15).</br>Although no survival benefit with angiotensin-II inhibitors was observed in this study, the</br>18 patients treated with an angiotensin-II inhibitor required half the steroid dose</br>compared to all other patients in the study (mean prednisolone dose of 29 mg per day</br>versus 60 mg per day), and this difference remained significant in multivariate analysis</br>(p=0.003).</br></br>A later retrospective study by the same group published in January 2016 (329) focused</br>specifically on the angiotensin-II receptor blocker class of drugs and their effects on</br>vasogenic edema in glioblastoma patients. In this study, 11 patients taking angiotensin-II</br>receptor blockers (ARBs) for hypertension were compared with 11 matched patients with</br>similar age, tumor size, and tumor location, but not taking medication for hypertension.</br>There was a significant 66% reduction in the FLAIR ratio in the patients taking ARBs</br>compared to the matched patients not taking ARBs. As FLAIR signal can represent either</br>tumor infiltration or vasogenic edema, the nature of the peri-tumoral FLAIR signal was</br>assessed with apparent diffusion coeffient (ADC) mapping. Nine evaluable patients taking</br>28</br></br>ARBs had a 34% reduction in ADC ratios compared to their matched controls not taking</br>ARBs, confirming the ability of this class of drugs to reduce peri-tumoral edema.</br></br>A 2015 study, also by the group in France, suggests angiotensin-II inhibitors (including</br>ACE inhibitors and ARBs) may also lead to superior survival outcomes (330). In this</br>study, 81 GBM patients were included. Seven of these patients were taking ACE inhibitors</br>and 19 were taking ARBs for hypertension. The 26 patients using angiotensin-II</br>inhibitors had increased progression-free and overall survival (8.7 and 16.7 months)</br>compared to the patients not taking these drugs (7.2 and 12.9 months). Use of</br>angiotensin-II inhibitors was a significant positive prognostic factor for both PFS and OS</br>in multivariate analysis.</br></br>A randomized phase 3 trial in France (NCT01805453) has recently completed</br>recruitment, and is testing the influence of losartan (an ARB) versus placebo on the</br>steroid dose required to control edema on the last day of radiotherapy. Another drug in</br>this class, telmisartan, has superior penetration into the central nervous system (331) and</br>may therefore be a better choice.</br></br>See Chapter 13 for a discussion of Angiotensin system inhibitors plus Avastin" contains invalid characters or is incomplete and therefore can cause unexpected results during a query or annotation process.

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