Scientist Discover the Cellular Roots of Graying Hair

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Findings Could Shed New Light on Malignant Melanoma

Few things about growing older are as inevitable and obvious as ''going gray,'' yet scientists have been unable to explain the precise cause of this usually unwelcome transformation.

In a report posted today on the Web site of the journal Science, researchers from Dana-Farber Cancer Institute and Children's Hospital Boston say they have found the cellular cause of graying hair while investigating the origins of malignant melanoma, the potentially deadly skin cancer.

The scientists traced the loss of hair color to the gradual dying off of adult stem cells that form a reservoir that spawns a continuous supply of new pigment-manufacturing cells, called melanocytes, that give hair its youthful hues. Not only do the non-specialized stem cells become depleted: They also progressively make errors, turning into fully committed pigment cells in the wrong place within the hair follicle, where they are useless for coloring hair.

The new findings won't lead to a scientific alternative to hair dyes any time soon, if ever, even if they do solve a longstanding puzzle about the underlying mechanism of graying. Of more interest to the researchers is the pattern of cellular signals that triggers the death of pigment stem cells, since melanoma is dangerous for the opposite reason - melanocytes proliferate uncontrollably to form tumors and are hard to kill with treatment.

''Preventing the graying of hair is not our goal,'' emphasizes David E. Fisher, MD, PhD, director of the Dana-Farber Program in Melanoma, and senior author of the Science paper. ''Our goal is to prevent or treat melanoma, and to the extent this research is revealing the life cycles of melanocytes, which are the cells that become cancerous in melanoma, we would love to identify a signal that would make a melanoma cell stop growing.''

Fisher and the report's lead author, Emi K. Nishimura, MD, PhD, also of the melanoma program, are in the Department of Pediatric Oncology at Children's Hospital Boston as well as at Dana-Farber. The second author, Scott R. Granter, MD, is a pathologist at Brigham and Women's Hospital.

The American Cancer Society expects about 55,100 people to be diagnosed with melanoma, the most serious form of skin cancer, in 2004, with an estimated 7.910 deaths. Melanoma can be cured when it is detected and treated early, but if the lesion penetrates deeply into the skin it is often fatal. Sun exposure is a major risk factor in the disease, which has been increasing in the past several decades.

Melanocytes, which manufacture and store the pigment that combines with hair-making cells called keratinocytes to color the hair, are specialized cells spawned by colorless melanocyte stem cells. These cells were discovered by Nishimura in 2002.

A pool of undifferentiated melanocyte stem cells resides in the hair follicle, and during the hair's grow-and-rest cycle, the stem cells give rise to color-making melanocytes that journey to the bottom of the hair follicle: That is where they tint the keratinocytes with the person's characteristic hue.

By studying mice at progressively older intervals, Fisher and his colleagues discovered that as the rodents aged and their hair began turning gray, the numbers of stem cells diminished in proportion to the loss of color. The scientists were surprised to observe that, at the same time and the same rate, differentiated, pigmented melanocytes were showing up in the follicle at the location where the stem cells resided.

Since they were in the wrong place, the pigmented cells likely did nothing to maintain the mice's hair color.

To see if the cells behaved the same way in humans, the investigators examined human scalp tissue taken at increasing ages, and determined that the same pattern occurred.

Since cell survival in general is influenced by an ''anti-death'' gene called Bcl2, Fisher's team analyzed mice lacking this gene. In a dramatic fashion, the mice lost their melanocyte stem cells shortly after birth and quickly went gray. It may be that people who gray prematurely have mutations that knock out Bcl2 activity, Fisher says.

''This tells us there is a requirement for Bcl2 in normal hair follicle cycling,'' adds Fisher. ''So the question is: what in the hair follicle is signaling the stem cells that is absent when aging occurs and the stem cells die off. Now we have a much more refined way of dissecting that signaling pathway in melanoma. Eventually we hope to tap into this death pathway, thereby using drugs to mimic the aging process, to successfully treat melanoma.''

The team also made mice lacking a gene, MITF that regulates Bcl2. These mice also went gray, but more gradually than did the mice that had no Bcl2. The loss of MITF activity, the investigators say, appears to be implicated in the mistaken differentiation of melanocyte stem cells that accompanies the stem cells' depletion. MITF, they conclude, seems to play a crucial role in maintaining the supply of stem cells within the hair follicle, and graying is the result of ''incomplete maintenance of melanocyte stem cells.''

The research was supported by the National Institutes of Health, and Nishimura received funding from The Shiseido Award in 2002 and The Charles A. King Trust of Fleet National Bank and The Medical Foundation.

Dana-Farber Cancer Institute is a principal teaching affiliate of the Harvard Medical School and is among the leading cancer research and care centers in the United States. It is a founding member of the Dana-Farber/Harvard Cancer Center (DF/HCC), designated a comprehensive cancer center by the National Cancer Institute.

http://www.exduco.net/news.php?id=1219
 

docj077

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hedgehog_info said:
Nice post....

BCL2 is a target of the hedgehog pathway.

And is increased in basal cell carcinoma. Not only that, but sonic hedgehog does not directly alter the transcription of the BCL-2 gene. This process takes place through Sonic Hhg activation of gli-1 within the pathway.

The use of Sonic Hhg as a treatment for any skin disease is a bad idea. In fact, it's the worst idea. You can use it for a limitied time at a limited dose, but if that individual has ever done damage to that area of skin with a sunburn or chemicals, they will develop cancer. Not only that, but if this substance is applied on a wide enough area of the scalp, there will be no way to stop its spread.

Again, bad idea. Growth stimulates will always be a bad idea when dealing with epithelial tissue. A lack of growth stimulation is not the underlying cause of male pattern baldness. There is already pro-cancer compounds in the scalp in the form of IGF-1. There is no need to apply more.
 

hedgehog_info

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And is increased in basal cell carcinoma.
Along with Pancreatic Cancer, Prostate Cancer, Breast Cancers, and Liver cancer to name few more.

Yes Gli2 activates Bcl2 gene.

The idea behind stimulating the Hh pathway for hair growth is not to generate new cells but kick the current ones into the growth phase.

I also don't think the drug itself is a mutagenic, but at high enough doses might cause cancer like growth.

A lack of growth stimulation is not the underlying cause of male pattern baldness.

A few people including P&G seem to think that hair follicle cycling requires a Hh pathway activation to get into the growth. The real problem will be how to stop the side effects.
 

docj077

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hedgehog_info said:
And is increased in basal cell carcinoma.
Along with Pancreatic Cancer, Prostate Cancer, Breast Cancers, and Liver cancer to name few more.

Yes Gli2 activates Bcl2 gene.

The idea behind stimulating the Hh pathway for hair growth is not to generate new cells but kick the current ones into the growth phase.

I also don't think the drug itself is a mutagenic, but at high enough doses might cause cancer like growth.

[quote:b0bdf]A lack of growth stimulation is not the underlying cause of male pattern baldness.

A few people including P&G seem to think that hair follicle cycling requires a Hh pathway activation to get into the growth. The real problem will be how to stop the side effects.[/quote:b0bdf]

So, you're absolutely sure that this pathway is somehow lacking in efficiency in people with male pattern baldness or how are you coming to such a conclusion that its application will be beneficial other than some results in mice or whatever? The SHh pathway in adults no doubt has a negative feedback mechanism to keep it under control. The loss of such feedback is probably an initiating event in many cancers. Who are you to say that this feedback inhibition won't simply be upregulated and overcome any application of a drug designed around SHh?
 

hedgehog_info

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Hi Doctor,

So, you're absolutely sure that this pathway is somehow lacking in efficiency in people with male pattern baldness or how are you coming to such a conclusion that its application will be beneficial other than some results in mice or whatever?

From what i understand the hair follicle is one of the few cells that continually express sonic hedgehog through out life. In most other places in the body it is only turned on when your tissue needs to repaired. There have been a few studies that used a mouse model of hair loss. According to the researchers they said that this animal strain has been extensively studied and characterized for hair cycling, hair loss, hair growth ect... After they applied an agonist (used to turn on the pathway) it grew hair in about 14 days with a one time dose.

They also looked at human scalp and confirmed that we humans also express this pathway when the hair needs to get kicked into the growth phase.

This agonist was going to be first used for people who lost hair due to chemotherapy. However, after curis licensed it to P&G they wanted to develop it for alopecia.

Curis has also stated that neuronal and hair follicles are the most sensitive to pathway activation. Obviously the formulation has to be perfect.

The SHh pathway in adults no doubt has a negative feedback mechanism to keep it under control. The loss of such feedback is probably an initiating event in many cancers.

Yes, one of the first targets the pathway upregulates is a gene called ptch, which is negatively regulates the Hh pathway. The regulation of this pathway is very complex and pretty poorly understood.

Who are you to say that this feedback inhibition won't simply be upregulated and overcome any application of a drug designed around SHh?

Well, the pharma companies are betting on a one time application will do the trick. Wyeth is hoping for a one time systemic application (for stroke) and P&G are hoping for a one time topical application. If you have skin cancer and you put this topical stuff on your head it is going to be like adding gasoline to a fire.

I honestly have more faith in the cancer aspect of this pathway. But like to see what people find about hair loss on this message forum.
 

abcdefg

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Why does science in fields like medicine give up on figuring out the relationships and correlations between all these seperate findings? it always seems to me that there are 20 different findings but no one ever attempts to piece them all together or come up with links among them.
 

docj077

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abcdefg said:
Why does science in fields like medicine give up on figuring out the relationships and correlations between all these seperate findings? it always seems to me that there are 20 different findings but no one ever attempts to piece them all together or come up with links among them.

You'd be surprised how much different things are when you're looking from the outside in.

Funding is granted for only certain experiments. Perhaps, no one has thought of it. What is more likely is that they just haven't been able to get the funding for it.
 

michael barry

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I would be extremely wary of the sonic hedgehog pathway until I seen it tested on both apes and humans and saw absolutely no increase in carcinomas over about a five year period afterwards.


If we "could" get hair back growing again.........................just the treatements currently available should be able to keep it on our heads. Im pretty convinced that finas plus spironolactone would more or less allow a young man to keep the hair he had for a few decades if he starts using it early enough.
 

Derelict

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that's very interesting about Mucuna pruriens "maybe" reversin grey hair, im going grey on the sides and would like to at least slow it down a little. Saw that it boost estrogen though, maybe negligible, might make my gyno worse, dunno.
 

John Difool

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"More commonly, Mucuna pruriens is used to promote muscle growth, increase strength and has been proven to raise levels of testosterone. It can help reduce menstrual discomfort in women and increase sperm motility in men. It can also help decrease psychological stress and increase sex drive.
 

Tom4362

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I wonder how the guys that posted in 2007 are doing right now
 
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