I would strongly encourage you to read through this blog and my own journey revealing the Inversion Pattern. Key moments were the Identical Diet experiment and the Extreme Cholesterol Drop experiment that I wrapped around the first presentation of my data for the Ketogains Seminar.
With this vital survey (5-8m of your time), we’re looking to gather a very large number of entries for our anonymised data pool. We’ll post graphs of the data in future articles and it will allow for strong information on some important decisions ahead.
Thank you in advance for your contribution to the data!
This will either be a single feature length documentary (90-120m) or a series of topic episodes (40-55m each)
I’ll be interviewing experts across the opinion spectrum. Pro lipid hypothesis, moderate, skeptic, liberal on statins vs conservative, etc.
We’ll explore:
History of cholesterol discovery
The #LowCarb movement and high “diet induced” #LDL
The science and data of risk: intervention, genetic, and observational
The two Triads, atherogenic dyslipidemia and ⬆️LDL+⬆️HDL+⬇️Triglycerides
And of course, we’ll be talking to many “Lean Mass Hyper-responders” (#LMHRs) across the world. Those who have gone low carb and have seen extremely high LDL and HDL, yet very low triglycerides.
Some are cautious, some confident, and some have taken steps to change.
I know many documentaries these days often tell one side of the story. When I say I hope to have experts across the opinion spectrum, I mean it! If you’ve followed my process for a while, you know I’m sincere in this endeavor. Each major position should be represented.
If a #LowCarb diet high in #SaturatedFat increases one’s cholesterol, even if it lowers many of their other heart disease risk factors, should it be avoided?
Do people with low #LDL live longer than those with high #LDL?
What can genetics tell us about the role of #LDL causality with heart disease? Are there any limitations in this form of science?
Do #LDL particles serve any benefit to the human body?
Is there any known context where high #LDL associates with low heart disease risk?
I can’t wait to ask these and many other questions on this journey of discovery. What better year to get a new perspective than 2020?
Lastly — I’ll be posting many updates on social media along the way. Use the hashtag #TheCCDoc to ping us.
We have some powerful news today – we now have it on strong authority that the followup time for the LMHR Measurement Project will be more than sufficient at one year, not five.
Spencer, Tommy, and I have been consulting many people both individually and together, including a very high level imaging expert. And we’re now confident progression of atherosclerosis for the LMHR population should be observable with CT Angiogram imaging at one year apart.
Needless to say, this is some very unexpected news. But I’d argue it is certainly more positive than negative. This does introduce a new slate of changes we’ll need to adjust for:
Our existing budgetary timing will be tighter. We have been seeking $2,000 per LMHR for this initial round of tests with the assumption we’d be raising the same amount for the second round in five years time. Given we’re now talking one year, the turnaround time will need to be much sooner.
However, with regard to (1) above, our high level expert has helped us figure out ways to save on the overhead per participant, but we can’t speak on that just yet. We now think we may be able to still keep the price to $2,000/each, but manage to cover both the first and second round testing.
This may change my own plans for the documentary and book. Given how close we are to having data in hand, it may be worth chronicling the effort in real time until it is wrapped, thus having a more compelling story for each medium given the big ending.
It’s pretty hard to express in words how seismic this news has been for us. Instead of a long stretch for half a decade once we officially start, we could instead be bringing forward powerful new data in just a twelve months regarding diet-induced high cholesterol and risk of atherosclerosis.
While I have historically used LDL-P and apoB metrics somewhat interchangeably, one advantage of measuring apoB over LDL-P is that apoB encompasses all of the potentially atherogenic particles: not just LDLs, but VLDLs, Lp(a), IDLs, and potentially chylomicrons. And this point has me relying more and more heavily on apoB today than on LDL-P in my patients and myself.
Understanding Remnants
Generally speaking, particles that are neither LDL nor HDL are considered “remnants” in the literature. (There’s some further distinction regarding Lp(a) and fully lipidated Chylomicrons in rare circumstance regarding this topic, but we’ll cover that in future article).
In other words, we have three categories of lipoproteins as labeled:
Remnant cholesterol, also known as remnant lipoprotein, is a very atherogenic lipoprotein composed primarily of very low-density lipoprotein (VLDL) and intermediate-density lipoprotein (IDL). Stated another way, remnant cholesterol is all plasma cholesterol that is not LDL cholesterol or HDL cholesterol, which are triglyceride-rich lipoproteins. Nonetheless, remnant cholesterol is primarily chylomicron and VLDL from which most triglyceride has been removed, such that each remnant particle contains about 40 times more cholesterol than LDL.
(Emphasis mine)
Which Lipoproteins have ApoB?
So which lipoproteins have this ApoB we’re talking about? That’s easy – basically every lipoprotein that isn’t an HDL*.
HDL particles (has no ApoB)
LDL particles (has ApoB)
Remnants (has ApoB)
* [If you want get technical, there’s some differences in opinion in the inclusion/exclusion of lipid-rich chylomicrons and Lp(a), with most leaning toward exclusion.]
Many people (myself included, originally) used LDL-P and ApoB interchangeably given the vast majority of “ApoB-containing Lipoproteins” in our bloodstream at any given time was likely to be LDL particles (LDL-P). My opinion on this definitely changed the more the Lipid Energy Model developed, because I could see how remnants uniquely told a story of the problem that LDL particles could not.
A Simple Boat Analogy
Imagine a fleet of cargo ships that are constantly being deployed and have two jobs:
Deliver goods, which takes 1 hour
Patrol and help out, which they do for 72 hours
You wouldn’t be surprised to see about 1 in 73 of these cargo ships having cargo and the rest being generally empty at any given time. Maybe some timing on launch or deliveries offsets this slightly so it’s more like 1 in 50 at times, or 1 in 100 other times.
Now let’s change it. What if you’re not seeing just one cargo ship full of cargo, you see 5. What does that mean?
You investigate further and find that there’s a reduced ability of these ships to deliver their cargo. They’re having a hard time completing their first job — the same job that should’ve been easy and take much less time on turnaround.
Maybe there’s a problem with the docks or rockier waters or the boats themselves. Regardless, you see more boats with cargo undelivered seems to associate with bad outcomes so you start to take notice.
Yet conversely, you notice that no matter how many more total boats you have, there seems to be very few bad outcomes when at any given time there are very few that have cargo — suggesting they are making their deliveries properly.
ApoB “Boats” Failing to Deliver
Most ApoB-containing Lipoproteins like chylomicrons and VLDL have a first job: to deliver their fat-based energy (triglycerides) to cells, and in normal circumstances it should happen very quickly (typically less than an hour). Then a large portion of VLDL will ultimately remodel to LDL particles and remain in the bloodstream for 2-4 days.
So let’s recreate our boat job list from above:
Deliver triglycerides, which typically takes less than an hour
Remain in the bloodstream (potentially immune/repair) for 2-4 days
But what do we commonly see in those who are obese, Type 2 Diabetic, or suffering other metabolic derangements?
High fasting VLDL
High fasting Triglycerides
And thus, high overall remnants
I posit the simple explanation in most of these cases is that there is a clearly reduced capability on the part of the existing VLDLs to make their deliveries (job #1), which matches up well with one being past the “personal fat threshold“. There’s little parking left for the triglycerides, so we see an accumulation of fat in tissues that aren’t designed to store it, such as ectopic fat.
Visceral fat is considered by many to behave as an ectopic fat depot, accumulating triglycerides (TG’s) when body fat storage needs exceed the capacity of subcutaneous fat depots to function normally
Talking LDL-P and ApoB with Attia
For those who managed to make it through the 3.5 hour podcast Peter and I had, you’ll note I kept bringing up this context often when I was outlining my dream request list on data. Peter was seeking to be helpful in talking about what datsets might have what I was looking for.
Here’s Peter:
The Quebec Heart Study, here I printed it up here. I mean, basically it’s showing it has nothing to do with the LDLC once you know the ApoB. Look at the risk.
After some further back-and-forth I managed to clarify better:
Triglycerides, HDL, and preferably LDLP. Now, there is an important distinction we’ve gotta make with ApoB, because ApoB can, in theory, also include remnant lipoproteins.
Peter agreeing on that note for what I’m looking for:
Thus far, I haven’t gotten ahold of dataset where I can do that stratification, but I certainly appreciate Peter’s interest in talking about it and his consideration in helping out. (An additional aside to Peter’s credit, he further offered to cover a visit to a National Lipid Association conference where I could’ve met with lipidologists on this very topic).
Are LDLs Getting the Blame for Remnants When Viewing only ApoB?
If one has high triglycerides, one almost certainly has high remnants, given they are triglyceride rich — much more so than LDL particles.
And given high triglycerides typically result in lower HDL (that’s a mechanistic discussion for another day), it’s understandable why this dysregulation would further associate with ectopic fat and yes, cardiovascular disease. (This profile is already recognized in the literature as Atherogenic Dyslipidemia)
Which brings us right back to the “Low Carb Cholesterol Challenge“. I believe the reason we’re having trouble finding studies where high LDL is shown to be atherogenic where HDL is high and TG low is that we are seeing low overall remnants, suggesting a more optimal lipid metabolism. One that is likely functioning well by comparison to one with low HDL and high triglycerides. (To date, we still haven’t had the challenge met.)
Moreover, it makes a lot of sense why one could have higher LDL due to longer residence time of remnants — thus having a higher marginal LDL for a negative reason. The tip off for whether this is the case being high VLDL and triglycerides. But this too is a hypothesis that I’m actively testing.
Final Thought
My larger point is that it is certainly my expectation that looking at ApoB by itself would likely show a greater association with cardiovascular disease given it lumps LDL-P with remnants. But I likewise expect we’d see a much stronger association with cardiovascular disease when looking at remnants without LDL-P.
…Addendum
I realized after posting this that I oddly forgot to mention the LMHR Measurement Project and how our current efforts will actually test the very hypothesis I mention above. Shame on me!
My primary costs are the many frequent and expensive blood tests I take for this research and data. Any size donation is appreciated. Thank you for your support!
Recent Comments