2015
DOI: 10.1002/ajmg.b.32313
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An angiotensin‐converting enzyme (ACE) polymorphism may mitigate the effects of angiotensin‐pathway medications on posttraumatic stress symptoms

Abstract: Angiotensin, which regulates blood pressure may also act within the brain to mediate stress and fear responses. Common antihypertensive medication classes of angiotensin-converting enzyme inhibitors (ACE-Is) and angiotensin receptor blockers (ARBs) have been associated with lower PTSD symptoms. Here we examine the rs4311 SNP in the ACE gene, previously implicated in panic attacks, in the relationship between ACE-I/ARB medications and PTSD symptoms. Participants were recruited from outpatient wait rooms between… Show more

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Cited by 41 publications
(31 citation statements)
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“…These results contribute to a growing body of evidence implicating central AT 1 R activity in the expression of conditioned fear and anxiety (Khoury et al, 2012, Marvar et al, 2013, Marinzalda Mde et al, 2014, Shekhar, 2014, Shekhar et al, 2006, Johnson et al, 2013, Nylocks et al, 2015, Saavedra et al, 2006), and identify CRFergic cells as a population on which AT 1 R antagonists may act to create these effects. Further, they indicate that the fear expression-attenuating effects of AT 1 R inactivation may be caused by a decrease in fear memory consolidation (i.e., the transfer of a memory from a short-term to a long-term store in a transcription-dependent manner)—rather than an inability to acquire conditioning—as AT 1a R (+/+) and CRF-AT 1a R (−/−) mice showed similar levels of freezing during auditory fear conditioning, but 24 hours later, CRF-AT 1a R (−/−) mice displayed significantly less overall freezing than wild types.…”
Section: Discussionmentioning
confidence: 53%
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“…These results contribute to a growing body of evidence implicating central AT 1 R activity in the expression of conditioned fear and anxiety (Khoury et al, 2012, Marvar et al, 2013, Marinzalda Mde et al, 2014, Shekhar, 2014, Shekhar et al, 2006, Johnson et al, 2013, Nylocks et al, 2015, Saavedra et al, 2006), and identify CRFergic cells as a population on which AT 1 R antagonists may act to create these effects. Further, they indicate that the fear expression-attenuating effects of AT 1 R inactivation may be caused by a decrease in fear memory consolidation (i.e., the transfer of a memory from a short-term to a long-term store in a transcription-dependent manner)—rather than an inability to acquire conditioning—as AT 1a R (+/+) and CRF-AT 1a R (−/−) mice showed similar levels of freezing during auditory fear conditioning, but 24 hours later, CRF-AT 1a R (−/−) mice displayed significantly less overall freezing than wild types.…”
Section: Discussionmentioning
confidence: 53%
“…However, previous studies by our lab (Khoury et al, 2012, Marvar et al, 2013, Nylocks et al, 2015) and others (Marinzalda Mde et al, 2014, Krause et al, 2011) suggest an important role for this receptor in fear-related pathologies such as PTSD. Our current data extend these findings by demonstrating for the first time that AT 1a Rs on CRF-expressing cells contribute to conditioned fear expression without affecting fear acquisition or baseline anxiety, locomotion, blood pressure, or heart rate.…”
Section: Discussionmentioning
confidence: 54%
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“…Notably, this reduction in PTSD symptoms was not observed with other classes of blood pressure medications, including ␤-blockers, calcium channel blockers, and diuretics. These clinical data support a role for the RAS in the regulation of stress response in individuals exposed to traumatic stress, and this finding was recently replicated (80). In this same study, genetic evidence for a single nucleotide polymorphism (SNP) in the ACE gene in this PTSD cohort was determined.…”
Section: The Renin-angiotensin System: Beyond Blood Pressure Controlmentioning
confidence: 61%
“…In this same study, genetic evidence for a single nucleotide polymorphism (SNP) in the ACE gene in this PTSD cohort was determined. Differential responses to ACE-Is and ARBs were found in those with the ACE intronic SNP (rs4311), as well as greater symptom improvements in PTSD among those with the CC genotype (80). Although speculative, it is possible that ACE genetic polymorphisms such as SNP (rs4311) may explain the varying individual propensities to develop CVD in this PTSD population.…”
Section: The Renin-angiotensin System: Beyond Blood Pressure Controlmentioning
confidence: 97%