Updated Research and Knowledge - Cutting Edge

It's not going to raise T levels when applied topically

I understand. So if i buy olive extract pills and put it in minox for example, i can reduces DKK-1 ?

Josh, have you got anything to update us with? I've decided to come off minox for a while - i'm sure it's what's causing the problems with my sinuses - and hoping the OL + EGCG mixture will at least help prevent further loss.

Chemical, what's your thoughts on OC?

I take a liquid Olive Oil leaf extract (contains Oleuropein) for general health and well being - works great especially if you are sick with a cold or flu. Do you think taking any of these items orally instead of or in addition to topically will help with hair loss? Amazing information on this thread - very educational - thanks.

If something dissolves completely does that mean its optimally absorbed into the correct layers of the scalp or dermal layer where it needs to be for the amount of time it needs to be to get used properly? Im not a chemist/biology person so I dont know if just mixing stuff together would ever even work topically. Everyone knows the skin is a very strong barrier to keep things out

If something dissolves completely in solution, it does not mean it will be delivered transdermally.

I think the PGD2 receptor involved in sleep is DP1, not the GPR44 receptor that affects hair growth and which seti blocks.


EDA2R, but not EDAR, is associated. No other study has been able to replicate the result of EDA2R being the most significant predictor -- maybe it's the case in Sardinians, somewhat of a genetic isolate, but not other populations? Still, EDA2R is one of the most linked genes, along with AR itself, a region on Chr20 near PAX1 and FOXA2, EBF1, TARDBP, and HDAC9.

According to this, AR -> PTEN normally (?), which inhibits the Pi3K -> Akt step. But supposedly PTEN is widely expressed throughout the body as a tumor suppressor. I'm not sure how that would affect the efficacy of increasing Pi3K if AR's inhibitory effect on the Akt pathway is one step downstream of Pi3K. Any ideas?



Interesting. I'll have to read more about EBF1, ERbeta, adipogenesis, and so on.

I have to disagree with you on Emu oil. Its not really being marketed by big companies for anything spectacular. In fact, I am. I've used it when I first started receding at 17 by itself and I saw modest regrowth after 2 months. Its got BetaSitosterol which you've just listed lol. Its not a scam, its a weak treatment for hair, however it does posses potent anti inflammatory effects which are proven.

The growth factors you've listed all inevitably end up increasing β-catenin to mediate their hair growth promoting effects.

IGF-1 inhibits GSKb3 which increases β-catenin
PGE2 inibits Axin which increases β-catenin
VEGF is increased by β-catenin
β-catenin also upregulates PDGF-A which is required for hair canal formation and anagen induction.

Regardless of how you activate β-catenin, you will see hair growth.

I'm intrigued by your usage of KGF. I will dig up some research on this soon.

Ecklonia cava is 40% fat soluble and water soluble (?) too which means it can be used in an oil based vehicle I take?

Unfortuneately:

Figure 3 shows 100 μg/mL did worse. Not promising.

Couldnt find any solubility info on ACT, nor Fo-Ti which actually has alot of potential to work seeing as it uses the shh pathway.

Baicalin (study) however, directly activates WNT and is quite solvent in ethanol with increasing temperature.

Gamma Linoleic Acid is very soluble in ethanol and can be mixed with oil:



So perhaps straight ethanol + GLA or ethanol + oil + GLA. I've got my hands on GLA (primrose extract) and I'm thinking of how to go about this.

Rosemarinus Officinalis isnt soluble in water but is soluble in solvents (ethanol?):



Also the main constituents of Rosemary are carnosol and carnosic acid:

Water soluble too apparently @1,425 mg/L at 25 deg C (est).

FeelsBad is correct. Someone pointed this out earlier and I made a post here.

Yes the Oleuropein will reduce DKK1. In fact, anything that has anti-inflamatory properties has the potential to reduce DKK1.

Will reply to other posts tomorrow and with some updates.

Fo-Ti seems to be solubale in distilled water:

Chemical, thank you very much for this.
I'm sure that I'm speaking on behalf of everyone that is not registered to this forum and follows this.
I Hope it will lead to something this time.

I'm not too familiar with the efficacy OC versus seti. I cant really comment on its topical vs oral intake effectiveness either. I dont see it being a huge problem taking it orally given that it doesnt interact with PGD2 itself, but I'm not a fan of systemic usage.

It could work but if does increase hair then you'd notice hair everywhere. OL and EGCG work differently when taken orally and I cant vouch for their oral effectiveness on hair growth. Theres not alot of research on oral supplements increasing scalp hair growth in AGA unfortuneately. You're much better off using them topically since they are quite soluble and have low-ish molecular weights.

Good question. Simply dissolving in a solution does not mean it will permeate the skin. The molecular weight in addition to solubility properties are a much predictor of topical absorption. This is a probabilistic model where complete absorption and equal tissue distribution is not guaranteed. Ethanol has the ability to strip the skin of lipids and enhance the absorption of molecules. Heres a post I made on minox/OL molecular weight and absorption.



I apologise, you are correct. It is indeed the DP1, so CRTH2 anatagonists shouldnt be a problem. I think I need you to correct mistakes in my analysis lol.

Two receptors for EDA were found that are specific for the two isoforms EDA-A1 and EDA-A2: EDAR and EDA2R, respectively. EDA-A1 and its receptor EDAR are capable of activating the NF-κB pathway and are implicated in hair growth. EDA2R is capable of activating the NF-κB pathway and also through TRAF3,6, JNK (c-Jun N-terminal kinase), which activates c-Jun. Mutations in EDA and EDAR give rise to ectodermal dysplasia, a clinical syndrome characterized by loss of hair, sweat glands, and teeth, whereas mutations in EDA2R do not. Recently, a preliminary report suggested that EDAR may influence hair thickness in Asians, A scan for genetic determinants of human hair morphology: EDAR is associated with Asian hair thickness.

EDA2R could influence the onset of AGA through the activation of the NF-κB pathway or by c-Jun, which has been shown to be critical for AR transactivation. Moreover, in adult mice, EDA2R is also expressed in the hair bulb and in differentiating hair matrix (Botchkarev and Fessing, 2005).

Indeed, its the EDA2R that is involved in AR transactivation. But the EDAR variant also activates nf-kb without negative effect on hair. It seems theres alot genes that can influence the AR and transactivation of AR via different mechanisms leading to increased nuclear translocation. A combination of these alleles that enhance AR be it subtly or directly, definitely have the ability to predispose individuals to AGA. The nf-kb pathway seems to have differential effects depending on its mechanism of activation? I think I'm missing something that doesnt explain why EDAR can increase hair thickness.


So this means in the presence of AR, anything that wants to activate AKT via PI3K will be unsuccessful. This includes IGF-1, shh, EGF (wiki). Beautiful diagram here: https://en.wikipedia.org/wiki/File:M...thway-v1.7.svg

But does this mean beard DPC do not inhibit PI3K via PTEN in response to AR activation? Apparently PTEN deficiency results in accelerated hair follicle morphogenesis and enhanced AKT(PKB) activation (study). Very interesting.

Heres some more research on ERb and hair.

So in females, ERb increases frontotemporal hair growth but inhibits in other areas?

Studies say that estrogen prolongs anagen but inhibits hair shaft elongation (in females). Perhaps ERb in the ORS is inhibiting proliferation, but ERa in the DPC is maintaining BetaCatenin. But Estrogen acts differently in frontotemporal regions? Females have a differential scalp response phenotype. Males start off as females in the womb, so what if Androgens exploit this localised response in a detrimental manner? This sets off the chain reaction whereby follicles release DKK-1 and TGF-Beta into the ECM affecting nearby follicles that arent fully susceptible to AR's effects.

Anyways, I want to know what role ERa has in male DPC. ERb can increase proliferation of existing hair, but does it secrete growth factors in a paracrine manner? Or does ERa promote WNT activation by itself in DPC to prolong anagen?

It can! This is excellent research SriHanuman. Unfortuneately I cant use this because I'm trying a different stack, so I wont be able to gauge its effectiveness. People who cant use minox might find fo-ti useful.

Thank you! We're uncovering so much research that I think it is already leading to something.

Update

Last week I increased the EGCG concentration totalling 12.5mg/ml. The hairs that I grew using minox + OL are 100% terminal. Really wasnt expecting results this fast. I'm seeing more tiny vellus hairs along nw1 hairline and the skin turning grey/green. My nw1/0 hairs grow sideways, as in they come out of the skin at very low degree angles. My nw0 is hairline is completely bald atm so it might be harder to regrow. I'm not sure if my aggressive micro-needling (3mm derma pen) last year has caused scarring. I hope not because I'd be devastated.

Bear in mind I'm using the MXOLCG once a day at night because of work and laziness, and Ketoconazole in the morning. During the weekends I use MXOLCG 3x day. If only I could use minox 3x a day everyday... I try to use Emu oil every two days, and I'll be adding the Gamma Linoleic Acid to the Emu oil (which has minox in it already). I'll be posting pics soon. I am tempted to use Rosemary but I'll wait.

I'm also going to ask the moderators to let me edit my first post so I can reorganise the research for people to find easily.

HEY Chemical thank you for what are you doing.

Can you do a summarise of your invention, like what exactly to use( what products it contains) , the concentration ,and how often to use like instructions on drughs???

Chemical , Can you please tell me how much EGCG and OL pills you are now using in a 60 MG bottle of minox ? I was dumping in one EGCG pill and a half pill of OL . Can you update the mix ?

There are a lot of new pages, sadly I did not find the courage to read everything ! ^^ So the idea to edit the first posts would be excellent.
Anyway I remember you said you don't take any anti DHT. According to you new hairs get thicker and potentially hold on thanks to EGCG but what about existing hair ? Do you apply the solution all over the scalp or only at temples ? Thanks for keeping us updated!

Thanks for the all the work Chemical and Brianboy. Ive purchased the supplies and keen to start soon.

Im already using seti in an etch/pg solution so keen to not add too much more ethanol to my scalp each day. That said, I want to ensure proper delivery to the follicles.

I have DMSO as well. Would a water/eth/pg/dmso be a good idea? What ratios are you both using?

I don't have any Keto to hand but I have some Dexamethasone, which apparently raises PGE2 and is an AA. Would adding that to the mix be too much? I see that you put your Keto on in the morning. Important to use it hours before the EGCG/OL mix?