The intervention strategy consisted of: community screening, detection, treatment, and control of cardiovascular disease risk factors by NPHWs (in collaboration with local physicians) guided by tablet-based simplified management algorithms, decision support, and counseling programs; provision of free locally available combination antihypertensive medications and a statin recommended by NPHWs, but supervised by local physicians; and support from a participant-nominated treatment supporter (friend or family member) to improve adherence to medications and health behaviors.

After enrollment in each community was completed, community clusters were randomized to either the intervention or usual care and followed for 12 months. Usual care included being given health literature on cardiovascular disease that was available locally and a recommendation to see their health care provider as usual.

In total, 14 (n=644) communities were assigned to the intervention and 16 communities (n=727) to usual care. Most of the participants (n=1,008; 73.5 percent) had a history of hypertension and were taking antihypertensive medications, but their blood pressure was not controlled.

Results showed a greater reduction in the primary endpoint of 10-year cardiovascular risk as measured by the Framingham Risk Score at 12 months in the intervention group vs. the control group (–11.17 percent vs. –6.40 percent), with a difference of change of –4.78 percent; p<0.0001. In the intervention group, there was a 34.2 percent relative reduction in the FRS estimate compared with baseline.

Greater absolute reductions were also seen in the intervention group compared with the control group for systolic blood pressure (11.45 mm Hg) and for LDL-C (15.85 mg/dL) (p<0.001 for both). More patients in the intervention group achieved blood pressure control, defined as <140 mm Hg systolic, than in the control group (69 percent vs. 30 percent; p<0.001). Medication adherence was higher with the intervention.

The community-based intervention was successful in urban and rural settings in two different countries and continents, with widely varying health systems and cultural backgrounds, wrote the authors, "which suggests our findings are widely applicable." They also noted the high degree of agreement in clinical decision-making between the NPHWs and physicians.

"Adoption of the HOPE 4 strategy could substantially enhance reduction in cardiovascular disease risk in those with hypertension, and in doing so help achieve the UN's General Assembly target that calls for a one-third reduction in premature cardiovascular disease mortality by 2030," said the researchers.

Schwalm JD, McCready T, Lopez-Jaramillo P, et al. Lancet 2019;Sept 2:[Epub ahead of print].

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Of 16,702 eligible patients in SwedeHF registered between May 11, 2000 and Dec. 31, 2016, only 1,599 (9.6 percent) had an ICD. Their mean age was 73 years and most (73 percent) were men. The propensity-matched study population consisted of 1,296 patients with an ICD and 1,296 patients without an ICD.

Patients who received an ICD were younger, more likely to be men and to receive guideline-directed medical therapy for HF. They were also more likely to have a history of ischemic heart disease, lower ejection fraction and a longer duration of HF, but less likely to have other comorbidities.

Results showed over a median follow-up of 2.69 years, there were 985 deaths (37.7 percent) in the matched cohort. For the endpoint of all-cause mortality, the risk of death was 12.7 percent and 16.9 percent in the ICD and non-ICD recipients, for an absolute risk reduction at one year of 4.2 percent (hazard ratio [HR], 0.73; p<0.01). At five years, the absolute risk reduction was 2.1 percent (HR, 0.88; p=0.04).

At one year, there were 737 cardiovascular deaths (28.2 percent). The one-year risk for cardiovascular mortality was 10.1 percent and 13.9 percent in the ICD ad non-ICD recipients, respectively, for an absolute risk reduction of 3.8 percent (p<0.01). At five years, this risk was 36.6 percent and 39.5 percent (HR, 0.88).

The short-term and long-term mortality benefit was consistent across subgroups, including patients with or without ischemic heart disease, men and women, patients younger and older than 75 years, those enrolled earlier vs. later in SwedeHF and thus receiving less or more contemporary treatment, and for patients with or without CRT.

"Our findings support the current recommendations and call for better implementation of ICD use in clinical practice," concluded Schrage.

In an accompanying editorial, Sana M. Al-Khatib, MD, MHS, and Fred M. Kusumoto, MD, FACC, comment that "the small number of patients who received an ICD may have magnified the apparent benefit of ICD due to unidentified covariates associated with risk of SCD; however, the authors used rigorous statistical methods including propensity score matching, and the results of the negative control analysis lend credibility to their findings."

While noting that the subgroups were too small for sufficient statistical power for robust comparisons, among other caveats, Al-Khatib and Kusumoto concluded the study "adds to the mounting evidence that ICDs are associated with improved survival in contemporary patients with HFrEF and highlights the need for strategies to improve their utilization."

Schrage B, Uijl A, Benson L, et al. Circulation 2019;Sept 3:[Epub ahead of print].

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Additionally, researchers noted that prescription rates of evidence-based secondary prevention therapies were high. They also highlighted substantial variations in clinical profiles across geographical regions. For example, patients in the Middle East had the lowest rates of current heart failure symptoms and lower extremity artery disease, along with the highest body mass index and highest prevalence of diabetes.

In contrast, patients from Asia had the lowest prevalence of prior MI, the highest rate of prior PCI, the highest rate of stroke, and the smallest body mass index and use of statins. Central and South America had the lowest rate of current smokers, prior stroke or angina, but the highest rate of hypertension.

Among the study limitations, CLARIFY reflects only middle- or high-income countries, making it impossible to extrapolate findings to large and important regions such as Africa and Asia where access to more advanced medical care is limited. Yet, Sorbets and colleagues say their findings are important given the substantial changes in the profile of CCS over the last decades.

Sorbets E, Fox KM, Elbez Y, et al. Eur Heart J 2019;Sept 3:[Epub ahead of print].

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Overall results showed participants with LDL-C genetic scores higher than the median had lower LDL-C levels (by 14.7 mg/dL) and an odds ratio (OR) of 0.73 for major coronary events. Similarly, participants with SBP genetic scores higher than the median had lower SBP (by 2.9 mm Hg) and an OR of 0.82 for major coronary events.

Participants in the group with both genetic scores higher than the median had LDL-C that was lower by 13.9 mg/dL, SBP that was lower by 3.1 mm Hg and an OR of 0.61 for major coronary events. Additional analysis showed exposure to increasing genetic risk scores and lower LDL-C levels and SBP was associated with dose-dependent lower risks of major coronary events.

While the findings are positive, the researchers caution that they "cannot be assumed to represent the magnitude of benefit achievable from treatment of these risk factors."

Ference BA, Bhatt DL, Catapano AL, et al. JAMA 2019;Sept 2:[Epub ahead of print].

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The study randomized 2,488 patients undergoing primary PCI with stent implantation to either a genotype-guided approach (n=1,242) or standard treatment (n=1,246) for 12 months. The two primary outcomes were net adverse clinical events (i.e, death from any cause, myocardial infarction, definite stent thrombosis, stroke or major bleeding) at 12 months and major or minor bleeding at 12 months. Patients carrying the CYP2C19*2 or CYP2C19*3 loss-of-function alleles in the genotype-guided group received ticagrelor or prasugrel, and noncarriers received clopidogrel.

In overall results, the primary combined outcome occurred in 63 patients (5.1 percent) in the genotype-guided group compared with 73 patients (5.9 percent) in the standard-treatment group. In the genotype-guided group, the primary bleeding outcome occurred in 122 patients (9.8 percent) compared with 156 patients (12.5 percent) in the standard-treatment group. Researchers noted there was no difference in major bleeding between both groups (2.3 percent in both); however, the between-group difference in the primary bleeding outcome was largely driven by a lower incidence of minor bleeding in the genotype-guided group.

Claassens, et al., highlighted "lower-than-anticipated incidence of the primary combined outcome, and the fact that genetic variation is not the only factor contributing to high platelet reactivity" among the trial's limitations. The also cautioned that a "strategy based solely on the CYP2C19 genotype may not be the most useful strategy for some patients" given there are additional polymorphisms of the CYP2C19 gene for which data are conflicting.

Claassens D MF, Vos G JA, Bergmeijer TO, et al. N Engl J Med 2019;Sept 3:[Epub ahead of print].

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