The Heart Stack and the Plan | Life Matters Faith

REMEMBER: I'm not a doctor. Or your doctor. This is informational and my personal experience. The statin part is a prescription drug — that means a doctor, not me, and not a website.

So, you've read about the peptides and the weight loss. GREAT. But losing 50 pounds and getting my blood sugar in line was only half the job. This page is about the other half — the part I almost got wrong. I came into this chasing muscle, and I walked out with a plan for my arteries that might matter a whole lot more. Here's the honest story of how I built my heart stack, the research behind every piece, the dosages, and how I actually take it day to day.

1) How this started: I went looking for muscle and found plaque.

My plan was a lean bulk — Testosterone plus Equipoise (EQ). I've been on TRT for 23 years, so the testosterone base is handled. I just wanted to add EQ on top and put on quality muscle, not fat. Simple. Then the thing I already knew, but had been quietly filing under "not serious yet," came back to the front of the line: I have coronary artery plaque.

Here's why that's not a footnote for me. My father died of a heart attack at 58. I'm convinced the same bad genetics that crashed my hormones at 42 — and made me start TRT that early — are the genetics that killed him. I don't get to pretend the plaque isn't there. And EQ, for all its upside, pushes on exactly the three things that decide whether plaque stays quiet or turns dangerous: it raises hematocrit (thicker blood), it can nudge blood pressure up, and it drags HDL down. That's the wrong direction on all three for a guy with my family history.

The honest turn: I didn't cancel the muscle plan. I sequenced it. Stabilize the heart first, get real numbers and imaging, THEN decide on the cycle from a known position instead of a guess. That decision is the whole reason this page exists. Background work first. Muscle hunting second.

2) The question that changed everything: can you actually MOVE plaque?

I asked a straight question — is there anything besides a prescription that actively reduces plaque? And at first the answer I got was the standard line: no, you can stabilize it but nothing really reverses it without drugs. I didn't buy it. I'd seen Dr. Kevin Ham, MD, talking about pomegranate, spirulina and natto helping people reduce arterial plaque. So I pushed back. Hard.

And here's the part I want you to take away more than anything on this whole page: when we actually searched the current research, the picture changed. The "nothing works" answer was overconfident and, frankly, was the kind of answer that could cost somebody real years. There IS legitimate clinical evidence that certain natural compounds move the needle. Small studies, yes. Needs more replication, yes. But real, and pointing the right way.

The lesson — make the AI SEARCH, don't trust its memory

This is the single most useful thing I learned. An AI answering from its training data is working off a frozen snapshot, and it'll hand you that snapshot with total confidence. The same AI, told to "search for current studies," pulls up the actual research and shows you the sources so you can check them yourself.

On a serious health question, those two answers can be the difference between "give up" and "here's a plan." So for anything that matters: don't accept the first confident answer. Tell it to go find the recent studies. Then read them. I use more than one AI and I make all of them show their work.

So I built a four-part stack, each piece backed by something we actually found in the literature, and each one checked against the others so they don't fight each other. Here's each one.

3) The foundation: the statin.

Rosuvastatin — Rosuprove-10 (plain, NO aspirin)

This is the engine of the whole stack, and it's the one prescription piece. My LDL sits in the normal range but toward the high side — and with known plaque, "normal" may not be low enough. The people who already have disease usually need to be pushed well below the standard cutoff. That's a conversation for my doctor, not a number I set myself.

Why rosuvastatin specifically

It's the most potent statin at lowering LDL per milligram, so I hit aggressive targets at a LOW dose — and lower dose means lower odds of side effects.
It's hydrophilic (water-loving), which means it penetrates muscle tissue less than the fat-loving statins like simvastatin or atorvastatin. That matters to me because I want to keep training.³
Its long half-life means if I ever turn out to be sensitive, I can dose every other day and still get real LDL reduction.
Bonus: grapefruit messes with the fat-loving statins but NOT the hydrophilic ones like rosuvastatin.

From Claude (Opus 4.8) — statins and the muscle myth

The muscle problem with statins is far smaller than its reputation. In blinded trials — where neither patient nor doctor knew who got the statin — muscle aches showed up at nearly the same rate in the placebo group. Most real-world "statin muscle pain," on careful rechallenge testing, turns out not to be caused by the statin at all. Genuine statin myopathy is real but uncommon, and true muscle damage (rhabdomyolysis) is rare.

The one side effect worth actually baselining is blood sugar — statins can nudge glucose up slightly. In my case that worry mostly dissolves, because the Retatrutide is driving my glucose down far more powerfully than a statin could nudge it up. Still worth knowing your A1C going in.

Why the PLAIN version and not Rosuprove-A: The "-A" version bundles in 75mg of aspirin.⁴ I'm running nattokinase (see below), and nattokinase plus aspirin stacks up the bleeding risk. So I deliberately chose plain Rosuprove-10 and I keep the components separate, where I control each one with my doctor. If aspirin ever makes sense, that's a decision we make on purpose — not because it came baked into a tablet.

My dose

Rosuprove-10 (10mg), taken at night. Statins do their work while the liver is busiest, which is overnight.

Muscle insurance (optional): If statin muscle aches ever show up, the two things with the best evidence are CoQ10 (100–200mg/day)⁵ and — already in my stack — spirulina, which has been shown to ease statin muscle symptoms. L-carnitine is the one extra worth a look⁷, partly for muscle and partly because it'll do double duty when I eventually run the cycle. Vitamin D gets recommended a lot, but a big randomized trial showed it does NOT prevent statin muscle pain.⁶ Skip it for that purpose unless you're actually deficient.

How LOW, not just "normal" — the number that does the real work.

This is the piece I didn't fully appreciate until I dug in, and it's the most important thing on this whole page. My LDL sits in the normal range — but on the HIGH side of normal. For a guy with plaque already on the wall, here's the hard truth: "normal" is the wrong target. The whole game is how FAR down you drive LDL, because plaque actually regressing tracks the SIZE of the drop, not just sneaking under some lab cutoff.

From Claude (Opus 4.8) — the magnitude point

In the GLAGOV trial, researchers measured coronary plaque directly with intravascular ultrasound — a tiny probe inside the artery, not a guess. A statin alone shrank plaque in 47% of patients. Adding harder LDL-lowering on top (a PCSK9 inhibitor) pushed that to 64% — and the regression tracked in direct proportion to how far LDL was driven down, with benefit continuing all the way to an LDL around 20 mg/dL, far below any standard guideline number, and no safety problems at those low levels.²

This isn't one small study, either. It sits on top of DOZENS of these ultrasound trials, which is exactly why the LDL-lowering lever is the most rock-solid part of the entire science of plaque.¹ Translation for me: the statin isn't there to nudge me into "normal." It's there to drive LDL down low and hold it there.

*** So when I sit with my doctor, "my LDL's fine, it's in range" is the WRONG frame for a man with plaque. The right question is: how low should we drive it, given what's already on the wall? For established plaque that usually means well UNDER the standard number, not just inside it. That's the conversation I'm having — and it's the one most people never think to ask. ***

The tool that actually scores it: a CAC scan.

You can't manage what you can't measure. For coronary plaque specifically, the key tool is a coronary artery calcium (CAC) scan — a quick, low-radiation CT that measures the calcified plaque in the heart's own arteries and gives you a single number.⁸ The higher the score, the more buildup, and the higher the risk of a plaque rupture down the road. That score is what tells a cardiologist how aggressive to get with everything else, and re-scanning later gives a real before-and-after instead of guessing off how I feel. It sees what no blood test can — which is the whole point, because feeling great and having plaque are two different measurements. This is the imaging I keep talking about, and it's worth more to my decision than any single blood marker.

4) Pomegranate juice — the one that started the argument.

Pomegranate Juice

This is the compound Dr. Ham mentioned, and it's the one that made me push back on the "nothing reverses plaque" line. When we dug into it, the evidence was genuinely there.

The research we found

A study led by Dr. Michael Aviram, published in Clinical Nutrition, followed 19 patients with severe carotid artery stenosis. After one year, the pomegranate group showed a significant reduction in carotid artery wall thickness — a key measure of atherosclerosis. That's actual regression, not just holding steady.⁹

Mechanism: pomegranate works largely by reducing LDL oxidation and inflammation — it targets the root machinery of how plaque forms, rather than "scrubbing" deposits.

Honest caveats: 19 patients is small. Wall thickness is a proxy measure, not a direct plaque-volume count. It hasn't been replicated at large scale. So it's promising and real, not gospel.

My dose & the timing rule

About 50 ml (a little under 2 oz) of real pomegranate juice in the morning. That's roughly the studied dose. Real juice, not a sugar drink with a picture of fruit on it.
Keep it AWAY from the statin. Pomegranate can slow the breakdown of rosuvastatin, which raises its blood level. There's a case report of muscle damage from the combo, though a crossover study found little real-world change.¹⁰ Either way, the fix is free and easy: statin at night, pomegranate in the morning. Separate them and you sidestep the whole issue while keeping both benefits.

The irony I like: some research suggests pomegranate plus a statin may actually boost cardioprotection and let you get the same effect at a lower statin dose. Cuts both ways — more effect can mean more side-effect risk too — so I just keep them time-separated and let my doctor watch the muscle markers.

5) Spirulina — the quiet workhorse.

Spirulina

This one surprised me with how much it pulls its weight, and it plays nicely with the statin instead of against it.

The research we found

Spirulina reduces key inflammation markers — hs-CRP, TNF-α, and IL-6 — and inflammation is one of the drivers of plaque progression and instability.¹² A dose of 2g/day for 12 weeks significantly lowered LDL in trials.¹¹ And higher daily doses have improved oxidative-stress and blood-pressure markers in people with hypertension — directly relevant to artery-wall health.

Best part for me: there are NO known interactions between spirulina and rosuvastatin, and research suggests spirulina actually eases statin-associated muscle symptoms¹³ while doing its own lipid-lowering work. So it's protecting my muscles AND my arteries at the same time.

My dose

Start at 1g/day to check tolerance, then work up to 3–4.5g/day over a few weeks.
Split it across two doses rather than one big hit.

Cheap, widely available here in the Philippines, real evidence, and it doubles as muscle insurance for the statin. Easy yes.

6) Nattokinase — and the dose almost everybody gets wrong.

Nattokinase

This is the one where the DOSE is everything, and it's where most people waste their money taking a fraction of what actually works.

The research we found — read the dose carefully

The largest clinical study of nattokinase enrolled 1,062 participants and gave 10,800 FU daily for 12 months. Result: significant reduction in carotid plaque size — a 36% plaque-area reduction — with improvement rates ranging from 66.5% to 95.4% depending on the person, and no adverse effects reported.¹⁴

The catch: the lower dose of 3,600 FU per day was found to be completely INEFFECTIVE for plaque. So the standard little 2,000 FU capsules most people buy are well below the range that actually moved plaque in the study.

Timing rule: nattokinase must be taken on an EMPTY stomach — about one hour before food or two hours after. Taken with food, the enzyme digests your food proteins instead of working on arterial fibrin, and you've basically wasted it.¹⁵

My dose

I sourced 4,000 FU tablets. Three a day = 12,000 FU, which clears the proven 10,800 FU threshold with a little margin — and the study showed no problems even at that level.
Spread across the day, each on an empty stomach — one before breakfast, one mid-afternoon between meals, one before bed away from food. That keeps active enzyme levels steady instead of one peak-and-drop.

The bleeding flag — this is why my statin is the plain one. Nattokinase thins the blood and reduces clotting. Stacked with an antiplatelet like aspirin, that bleeding risk climbs.¹⁶ That's the whole reason I refused the aspirin-combo statin. Nattokinase alongside plain rosuvastatin: fine. Nattokinase plus aspirin: a real conversation with the doctor before you ever combine them. I just don't combine them.

One more for me personally: my blood pressure already runs LOW since the weight loss and the Reta. Nattokinase nudges BP down a touch too. So I keep an eye on it. Probably a non-issue at my activity level, but it's on my radar.

7) The foundation under all of it: food and movement.

Here's the part I almost left off this page — and that tells you something, because it's the part everybody skips and it might be the most important of all. Those four things above don't work floating in space. They sit on a foundation. If the foundation's rotten, the whole stack is just expensive damage control. The foundation is what I eat and how I move.

I'll be straight: I came at this hunting for compounds and a pill, because that's the fun part. But the honest truth is the evidence for diet is STRONGER than the evidence for three of my four supplements. That's not a knock on the stack — it's a reminder of what's actually doing the heavy lifting.

From Claude (Opus 4.8) — food moves plaque too

Both the Mediterranean and the DASH eating patterns are tied to slower progression of atherosclerosis and noticeably less plaque buildup — people who eat this way carry less coronary calcium.¹⁷ The mechanism is the same root machinery the supplements poke at: plenty of fruit, vegetables, whole grains, fiber and good fats lower LDL, cool down inflammation, and bring blood pressure down — and those are the three levers that decide whether plaque grows or stays quiet.

Fiber specifically — oats, beans, vegetables — pulls LDL down. Cutting saturated fat and swapping in unsaturated fats (olive oil, nuts, fatty fish) does the same. None of this is exotic. It's just consistent, and it works.

*** The movement half I've actually got covered — pickleball, 6 to 8 games, three times a week. That's not nothing. Staying active is one of the better-proven things you can do for the artery lining, and it's probably part of why I'm in decent shape DESPITE the plaque. The food half is where I have to stay honest, especially now that I want to eat more to build muscle. And two more boring levers that matter as much as anything in a bottle: don't smoke, and keep blood pressure and blood sugar in line. My BP runs low and the Reta has my sugar handled, so I'm in good standing there — but for most people, THAT'S the real fight, not which supplement to buy. ***

Bottom line: no supplement and no statin undoes a bad diet eaten sitting still. The stack works because it sits on a foundation — not instead of one.

8) The daily routine — how it all actually fits together.

On paper it looks like a lot. In practice it's four things slotted into the day around one simple rule: the statin and the pomegranate stay on opposite ends, and the nattokinase stays away from food. Here's my day:

When	What	Why
Morning (before breakfast)	Pomegranate juice (~50 ml) 1 × Nattokinase 4,000 FU Spirulina (dose 1)	Pomegranate is far from the night statin. Nattokinase on an empty stomach before food.
Mid-afternoon (between meals)	1 × Nattokinase 4,000 FU Spirulina (dose 2)	Empty-stomach window so the enzyme works on fibrin, not lunch.
Evening (before bed, away from food)	1 × Nattokinase 4,000 FU	Third dose keeps enzyme levels steady through the day. 12,000 FU total.
Night	Rosuprove-10 (rosuvastatin 10mg)	Statin works best overnight while the liver is busy. Far from the morning pomegranate.

The simple version to memorize: Statin at night. Pomegranate in the morning. Nattokinase ×3, always on an empty stomach. Spirulina split morning and afternoon. That's the whole stack.

9) The plan from here — and where the muscle comes back in.

This isn't a "take it and forget it" thing. The whole point was to build a known, stable starting position. So here's the sequence I'm actually running:

Run the stack for about 2 months. Rosuvastatin moves lipids fast — meaningful LDL reduction usually shows in 4–6 weeks — and the other three are building their effects in parallel.
Then bloodwork. A real before-and-after. My baseline a month ago was strong — I got summarized with the numbers of a (non-athletic) 30-year-old, everything in normal range. But that was BEFORE any of this, and it can't see inside the artery wall. The recheck shows me direction of travel.
And imaging. This is the piece bloodwork can't replace. For coronary plaque the key tool is the coronary artery calcium (CAC) scan I described above — it scores exactly what's on the artery walls — and a carotid ultrasound can add a look at the neck arteries. Either way I get a direct measurement to compare against later. I'm lucky — I'm five minutes from a teaching hospital here in Dumaguete with real cardiology capacity, and doctors here measure and discuss instead of preaching. I'll have a cardiologist who knows the full picture.
THEN — and only then — I reassess the Test + EQ cycle. If the lipids are down, BP stable, and imaging shows the plaque holding steady or regressing, I'll weigh the cycle against what the picture looks like THEN, with a cardiologist who knows everything I'm taking, named out loud. If it looks good and stable, I'll probably risk it. If it doesn't, I won't. That's the difference between an informed risk and a blind one.

*** I want to be straight about something. The AI I built this with did NOT talk me out of the cycle, and it didn't catastrophize. It gave me the real read for MY situation — known plaque is the profile where adding EQ is hardest to justify — and I'm the one who decided to do the heart work first. That's how this should go. Straight information, my decision. And the foundation I'm building now is exactly what makes the cycle a more reasonable risk later, not less. ***

Same as always: check every bit of this with an AI — and make it SEARCH current studies, don't trust its memory — and run it past a doctor who follows your blood panels. It's much cheaper here in the Philippines, and the doctors don't treat you like a child for taking charge of your own health.

DISCLAIMER — One more time:
The above is for education and my personal experience. I'm not a doctor. Just a guy. The statin is a prescription — get it from a doctor, properly, with bloodwork. Use your judgment and your doctor. I'm giving no medical advice. Just information.

Take care of your heart. You only get the one. Have a great day and life!

Show My Work — References & Notes

I said make the AI search and show its work, so here it is. Every claim above traces to something you can check yourself. Where the evidence is thin, mixed, or just one study, I say so on purpose — that's the honest part, and it's where you and your doctor earn your keep. Studies are linked; read them.

Statins shrink and stabilize plaque, in proportion to how much LDL drops. Prior intravascular-ultrasound trials show statins slow progression or induce regression of coronary disease in proportion to the magnitude of LDL-C reduction. Note: full "reversal" isn't achievable; stabilizing plaque so it's less likely to rupture is most of the benefit. Cleveland Clinic newsroom — link; Cleveland Clinic Journal of Medicine summary — link.
GLAGOV trial — driving LDL lower is what moves plaque. Nicholls SJ et al., JAMA 2016;316:2373–2384. 968 patients, IVUS, 78 weeks: adding a PCSK9 inhibitor to a statin produced plaque regression in ~64% of patients vs ~47% on statin alone, with regression in direct proportion to LDL levels — benefit continuing down to ~20 mg/dL (mean LDL on the combo ~36.6). Cleveland Clinic Journal of Medicine — link; JACC: Cardiovascular Imaging (regression "to LDL-C levels as low as 20 mg/dL") — link.
Rosuvastatin is potent and hydrophilic. Rosuvastatin 10 mg lowered LDL ~45% (61 mg/dL) in 8 weeks (NewStaR4G, J Clin Med 2020) — link. Hydrophilic statins penetrate muscle less than lipophilic ones, though a muscle transporter (OATP2B1) can still admit some — so "less," not "zero" — link.
Rosuprove-10 (plain) vs Rosuprove-A (with aspirin). Rosuprove-10 = rosuvastatin 10 mg only; Rosuprove-A = rosuvastatin + aspirin (10/75 or 10/150). Johnlee Pharmaceuticals, India. Rosuprove-10; Rosuprove-A 10/75.
CoQ10 for statin muscle symptoms — evidence is genuinely mixed. Some analyses show benefit (JAHA 2018 meta-analysis; a 2024 systematic review found 4 of 7 RCTs positive — link); others found none (Banach et al., Mayo Clin Proc 2015 — link; Taylor et al., Atherosclerosis 2015 — link). Low-risk to try; not a sure thing.
Vitamin D does NOT prevent statin muscle symptoms. VITAL substudy (Hlatky et al., JAMA Cardiology 2023): 2,083 new statin users, muscle symptoms in 31% of both the vitamin D and placebo groups — the first randomized trial on this. Smaller/observational studies hinted at benefit in deficient patients, but the RCT found none overall. PubMed; Northwestern summary.
L-carnitine / selenium for statin muscle — limited. Plausible mechanisms and some interest, but the human data are thin and no major cardiology guideline recommends routine use. Treat as optional/experimental, not established.
The CAC scan as the tracking tool. Coronary artery calcium is highly specific for coronary atherosclerosis and a guideline-endorsed risk tool; scores run 0 (none), 1–10 (minimal), 11–100 (mild), 101–400 (moderate), >400 (severe), with >100 (certainly >300) prompting more aggressive treatment. JACC review — link; National Lipid Association statement — link.
Pomegranate juice and carotid plaque — promising but mixed. Aviram M et al., Clinical Nutrition 2004;23(3):423–433: 19 patients with carotid stenosis; the 10 who drank 50 mL/day cut carotid intima-media thickness up to 30% at one year (vs +9% in controls), with lower BP and LDL oxidation — link. BUT a larger RCT (Davidson et al., Am J Cardiol 2009; 289 subjects, 240 mL/day, 18 months) found NO significant difference in CIMT progression — link. Small positive trial, larger null trial: real, not settled.
Pomegranate–statin timing is a low-cost precaution. The classic juice–statin interaction works through the CYP3A4 enzyme and chiefly affects lipophilic statins (atorvastatin, simvastatin); rosuvastatin is minimally CYP-metabolized, so any pomegranate effect on it should be small. Statin at night, juice in the morning, and the question is moot. Rosuvastatin interaction overview — link.
Spirulina improves the lipid profile (modestly). GRADE meta-analysis of 20 RCTs (1,076 participants): significant reductions in LDL, total cholesterol and triglycerides, and higher HDL — link. A separate meta-analysis found the LDL drop not statistically significant — so the effect is real but modest and variable. Studied doses 1–8 g/day, usually ~3 months — cardiometabolic review.
Spirulina lowers inflammation markers. Meta-analyses show reduced CRP (7 trials — link) and reduced CRP, IL-6 and TNF-α (22 studies, 5,385 participants — link).
Spirulina easing statin muscle injury — animal evidence only. A 2025 rat study found spirulina reduced statin-related muscle-damage markers and preserved muscle structure (Abdelhady et al., Med Sci 2025) — link. This is preclinical (rats), not yet shown in humans. No established direct spirulina–rosuvastatin interaction.
Nattokinase and plaque — one large study, dose-dependent. Frontiers in Cardiovascular Medicine 2022, 1,062 participants (avg age 67.5): 10,800 FU/day for 12 months reduced carotid plaque area ~36% and intima-media thickness ~21.7% (improvement 66.5–95.4%); 3,600 FU/day did nothing; well tolerated — link. Caveats: a single retrospective study, conducted in China, with tablets supplied by the manufacturer — it needs independent replication. (It actually found aspirin co-administration synergistic; I avoid aspirin for the separate bleeding reason in note 16.)
Nattokinase timing — and a real dose disagreement. For fibrinolytic effect, take on an empty stomach (30–60 min before food or 2+ hours after); food competes for the enzyme — link. Important: many clinicians hold the clinically studied/safe range is ~2,000–4,000 FU/day and that higher isn't proven to add benefit and may raise bleeding risk — directly at odds with the 10,800 FU plaque study (and my 12,000 FU). I'm following the plaque study; the conservative camp would not. Settle this with your doctor. link.
Nattokinase bleeding risk — the reason I keep aspirin off. Nattokinase has blood-thinning (fibrinolytic + antiplatelet) activity that adds to aspirin and anticoagulants; Memorial Sloan Kettering flags excess bleeding with daily aspirin, and case reports include cerebellar hemorrhage on aspirin + nattokinase. Stop it 1–2 weeks before surgery. MSK — link; interactions/case reports — link. (An automated drug-checker shows "no interaction," but the pharmacology and case reports say otherwise — the interaction is real.)
Diet and movement are the foundation. High DASH-diet adherence is linked to far less coronary calcium (MASALA cohort: 41% lower odds of CAC >100, stronger in men) — link; fiber and swapping saturated for unsaturated fat lower LDL. Most of this is associational and about slowing/less buildup; strong "reversal" evidence is limited and comes mainly from intensive lifestyle programs.

How this list was built: I had the AI run live web searches for each compound and claim, pulled the primary studies where possible (journals, PubMed, the manufacturer), and kept the caveats in plain sight. None of it replaces your own doctor and your own bloodwork.

← Back to Health Menu