Up - regulation of androgen receptor by heat shock protein 27 and miR - 1 induces pathogenesis of androgenic alopecia
- Thread starter jamesbooker1975
- Start date
- Reaction score
- 211
- Reaction score
- 442
f*** me. I checked the literature and Sauna increases HSP27 and Mir-1 at least temporarily... but it is supposed to be good for health in many ways. I go to sauna literally everyday but I value hair more than anything else.
In here, they analyzed people who die in sauna from heat exposure, and tissues present high quantities of HSP27 staining in the samples (creepy study ngl): https://www.researchgate.net/figure...ue-positive-HSP27-staining-200_fig3_348485115
Im confused and paranoid now cos my regime is hardcore. But idk, maybe having a temporary raise shouldn't matter enough, like Finns dont seem to bald more than rest of europe and they sauna everyday.
But would suck to nocebo myself into some unproven theory lmao
In here, they analyzed people who die in sauna from heat exposure, and tissues present high quantities of HSP27 staining in the samples (creepy study ngl): https://www.researchgate.net/figure...ue-positive-HSP27-staining-200_fig3_348485115
Im confused and paranoid now cos my regime is hardcore. But idk, maybe having a temporary raise shouldn't matter enough, like Finns dont seem to bald more than rest of europe and they sauna everyday.
But would suck to nocebo myself into some unproven theory lmao
- Reaction score
- 442
I doubt a normal hot shower or sunny day will increase much HSPs. For heat shock proteins to go up you must be really really hot (death tier level if prolonged) like a sauna.
- Reaction score
- 194
Cyanidin 3-O-arabinoside suppresses DHT-induced dermal papilla cell senescence by modulating p38-dependent ER-mitochondria contacts
Cyanidin 3-O-arabinoside suppresses DHT-induced dermal papilla cell senescence by modulating p38-dependent ER-mitochondria contacts - Journal of Biomedical Science
Background Androgenetic alopecia (Androgenetic Alopecia) is a genetic disorder caused by dihydrotestosterone (DHT), accompanied by the senescence of androgen-sensitive dermal papilla cells (DPCs) located in the base of hair follicles. DHT causes DPC senescence in Androgenetic Alopecia through mitochondrial dysfunction. However...
jbiomedsci.biomedcentral.com
AR transcription activity was increased by about 250% with DHT, but significantly decreased to control levels with C3A pretreatment (Fig. 2E). DHT-bound AR interacts with heat shock protein 27 (HSP27). When phosphorylated HSP27 is bound with AR, it translocates into the nucleus [28, 29]. Therefore, we assumed that C3A would inhibit AR nuclear translocation by affecting the interaction between AR and HSP27. We found that DHT increased the phosphorylation of HSP27, which was decreased with C3A pretreatment (Fig. 2F)
- Reaction score
- 194
Effects of dihydrotestosterone on rat dermal papilla cells in vitro
DHT also induced the phosphorylation and nuclear translocation of heat shock protein 27 (HSP27). Moreover, DHT decreased the levels of total and nuclear β-catenin, an important regulator of hair growth and proliferation, while lithium chloride, a glycogen synthase kinase-3β inhibitor, attenuated the DHT-induced downregulation of the β-catenin level. On the other hand, DHT increased the phosphorylation of mammalian target of rapamycin (mTOR), a regulator of proliferation, in immortalized DPCs. These results illustrate that DHT could shorten the duration of the hair growth cycle by initiating cell-cycle arrest, downregulating the β-catenin level, and upregulating the TGF-β/Smad and HSP27 level, whereas activation of mTOR by DHT could attenuate the inhibition of hair growth cycle in immortalized DPCs.
Effects of dihydrotestosterone on rat dermal papilla cells in vitro
Androgenetic alopecia involves the action of dihydrotestosterone (DHT) on dermal papilla cells (DPCs) that line the base of the hair follicle. However…
- Reaction score
- 194
Membrane-associated androgen receptor (AR) potentiates its transcriptional activities by activating heat shock protein 27 (HSP27)
Membrane-associated androgen receptor (AR) potentiates its transcriptional activities by activating heat shock protein 27 (HSP27)
The androgen receptor (AR) is a ligand-activated nuclear receptor that plays a critical role in normal prostate physiology, as well as in the developm…
- Reaction score
- 997
Then , DHT is good or bad for hair?
- Reaction score
- 442
So it seems its more DHT/high AR activity is raising HSP27 than the other way around? You guys are surely panicking me about my heavy sauna use lolMembrane-associated androgen receptor (AR) potentiates its transcriptional activities by activating heat shock protein 27 (HSP27)
Membrane-associated androgen receptor (AR) potentiates its transcriptional activities by activating heat shock protein 27 (HSP27)
The androgen receptor (AR) is a ligand-activated nuclear receptor that plays a critical role in normal prostate physiology, as well as in the developm…www.sciencedirect.com
HSPs do increase before catagen
- Reaction score
- 342
Anyone thinking of trying this? Paper says low sides and toxicity, it's a natural compound so maybe procurable and cheap... Seems it works differently than other AAs, so could be synergistic.Cyanidin 3-O-arabinoside suppresses DHT-induced dermal papilla cell senescence by modulating p38-dependent ER-mitochondria contacts
Cyanidin 3-O-arabinoside suppresses DHT-induced dermal papilla cell senescence by modulating p38-dependent ER-mitochondria contacts - Journal of Biomedical Science
Background Androgenetic alopecia (Androgenetic Alopecia) is a genetic disorder caused by dihydrotestosterone (DHT), accompanied by the senescence of androgen-sensitive dermal papilla cells (DPCs) located in the base of hair follicles. DHT causes DPC senescence in Androgenetic Alopecia through mitochondrial dysfunction. However...
AR transcription activity was increased by about 250% with DHT, but significantly decreased to control levels with C3A pretreatment (Fig. 2E). DHT-bound AR interacts with heat shock protein 27 (HSP27). When phosphorylated HSP27 is bound with AR, it translocates into the nucleus [28, 29]. Therefore, we assumed that C3A would inhibit AR nuclear translocation by affecting the interaction between AR and HSP27. We found that DHT increased the phosphorylation of HSP27, which was decreased with C3A pretreatment (Fig. 2F)