来自于John Harris 博士最新报道，呼吁世界上更多人关注和支持白白研究！

heavyrain78

发布日期:2018年11月27日，星期二
发件人:约翰·e·哈里斯
标签:白癜风，白癜风研究，白癜风治疗

我写这篇文章是为了响应许多令人兴奋和慷慨的请求，以帮助支持我们寻找白癜风治疗方法的研究工作。世界各地的读者主动向我伸出援手，他们和我们一样，对改善数千万白癜风患者的生活充满热情，这让我感动。作为回应，我们建立了一个用户友好和安全的方法捐赠支持我们的工作。在博客的最后有一个链接可以做到这一点。我还将概述我们在捐助者支持下迄今所做的工作，并告诉你们，如果我们有足够的资源，我们将来想去哪里。你可以帮助!

在过去的8年里，我们的团队从2名科学家(我加上一名研究技术员)发展到现在的15多名，由来自世界各地的学员组成，他们都在为白癜风患者寻找更好的治疗方法贡献他们的专业知识和热情。我们吸引了来自美国、中国、日本、埃及、巴基斯坦等地最优秀、最聪明的人才与我们合作，实验室每天都充满了新的想法和兴奋。他们知道他们的工作是重要的，他们非常认真地对待他们的任务。与此同时，我们彼此取乐、取长补短，欣赏彼此的差异，也在共同的事业中找到了同志情谊。

我们发起了一个重要的项目大约4年前那是不支持的国家卫生研究院(NIH)或其他政府资助一个项目,该项目是由私人慈善和关注学习为什么成功治疗白癜风的地方回到相同的位置后停止治疗。在这些研究中，我们发现自体免疫记忆T细胞在皮肤中形成并重新激活斑点，我们发现这些细胞依赖于在皮肤中表达的一种叫做IL-15的蛋白质。长话短说，当我们用一种新的治疗方法阻断这种蛋白质时，我们能够移除那些记忆细胞，并观察到白癜风小鼠中这种疾病的长期逆转。人体研究反映了我们在老鼠身上的观察结果，我们很高兴地报告，我们已经得到NIH的资助，将于2019年夏天开始在病人身上进行一项临床试验，以测试这种疗法。你可以在这里阅读更多关于这项研究的内容、结果和影响:

https://www.umassmed.edu/vitiligo/blog/blog-posts1/2018/08/science-translational-medicine-journal/

https://theconversation.com/new -处理-在- - -适合毁容-皮肤疾病白癜风-100058

我们还很幸运地得到了私人慈善机构的支持，他们支持了一个新项目，旨在发现皮肤中存在的免疫细胞，这些细胞要么引发疾病，要么抑制疾病。为了做到这一点，我们使用了一种非常新的，但是很昂贵的技术，叫做单细胞RNA测序，并将这种技术直接应用于我们从受感染的患者皮肤中获得的细胞。我们最近开发了一种新的方法，利用吸水泡对患者皮肤进行取样，这为这些研究提供了一个全新的机会，我们开始这个项目时，只观察了2-3名白癜风患者的皮肤，以确定这项尖端技术是否适用于这一目的。这项由支持者出资的早期数据非常令人兴奋，使我们能够从NIH获得125万美元的资助，将我们的研究扩大到更多的患者。到目前为止，我们分析了许多白癜风患者和健康对照组的皮肤，得到了惊人的分辨率和令人兴奋的结果。我们现在面临的“好问题”是，我们有更多的想法来开发更好的治疗方法，我们需要加倍努力去实现它们，这将需要更多的支持和资源来有效地做到这一点。

我们相信，这些研究将改变我们对免疫系统如何引起白癜风的理解，而这种疾病的“治愈”可能会在我们已经收集的数据中找到。然而，我们现在必须进行更多的研究，以在这些数据中找到导致治愈的关键因素。目前，这有点像大海捞针，我们真的需要“所有动手的平台”来完成这项工作。我们最终将实现这一目标，或者与我们目前的科学家小组长期合作(20-30年)，或者与一个更大的团队和扩大的资源合作(5-10年)，使我们能够更有效、更迅速地完成这一目标。

我们下一步的工作重点包括聘请科学家加入这个团队，他们将负责使用现有的数据，并从中提炼出最有希望的治疗目标。充分的支助也将使我们能够为这项工作使用现有的最佳工具，这些工具往往超出我们目前的预算。如果你想成为我们正在做的事情的一部分，请考虑点击链接，并捐赠任何你可以帮助我们。我将定期写信告诉你我们的进展，希望有一天我们能找到治疗方法，告诉你这个好消息。加入我们吧!  
个人认为这才是治疗白白的最大期盼！

karonka

真正在造福人类的人

DAZHI

John E. Harris, MD, PhD, and colleagues have made a promising discovery that could lead to therapies for vitiligo with longer-lasting effects, according to new research published in Science Translational Medicine on July 18.

Vitiligo develops when T cells attack and destroy skin cells, destroying pigment and leaving patches of the skin unpigmented. There are effective treatments for the condition, but the depigmentation returns in 40 percent of cases within the first year after treatment. Researchers have hypothesized that this recurrence could be due to the acti** of a type of T cell called “resident memory T cells” (or TRMs). However, translating these findings into a more durable treatment for vitiligo has been challenging.

“Patients are a huge motivation for what we research,” said Dr. Harris, associate professor of dermatology and director of the UMass Medical School Vitiligo Clinic and Research Center. “Ultimately, we want to give vitiligo patients treatments that last a long time.”

In the paper, Jillian Richmond, PhD, instructor in dermatology and a member of the Harris lab, and colleagues analyzed lesi** from vitiligo patients and found they contained TRMs that express components of a receptor for interleukin-15 (IL-15), an immune signaling molecule. Researchers administered an antibody that targets the IL-15 receptor for two weeks to mice with established vitiligo, and observed that the treatment restored pigmentation in the mice over the next two months.

“We are working with the Immune Tolerance Network, an NIH-supported national funding agency formed to conduct mechanistic studies that address immune tolerance in humans, to develop a clinical trial to determine whether targeting T cells could represent a viable therapeutic strategy for vitiligo patients,” Harris said.

The research was supported in part by the NIH’s National Institute of Arthritis and Musculoskeletal and Skin Diseases and the National Institute of Allergy and Infectious Diseases.

这是消息

15065070538

这是什么，不懂英文啊！

DAZHI

http://stm.sciencemag.org/content/10/450/eaam7710
这是原论文网址 全部浏览要50美元

DAZHI

New treatment in the works for disfiguring skin disease, vitiligo

John Harris
andreonegin/shutterstock.com
I am a physician-scientist and director of the Vitiligo Clinic and Research Center at the University of Massachusetts Medical School and I’ve witnessed my patients’ suffering and depression. Some are so ashamed of how they look; they refuse to leave their homes in daylight, they quit their jobs, and they lose relati**hips. Some of those afflicted with vitiligo have committed suicide.

I began studying vitiligo in 2008 because this devastating condition affects about one percent of all people – over 75 million worldwide – and patients deserve better treatments. In a recent report published in Science Translational Medicine we describe a new therapy that is showing particular promise in mice with this disease.

Your skin has a memory


Existing treatments such as topical steroids and light therapy, which are used “off-label” because they have not been FDA-approved to treat vitiligo, can be effective for patients. These treatments reverse the disease by stimulating brown spots to appear around hair follicles within the affected white patches of skin. As these brown spots increase in number and size they merge until the white patch is replaced with normal skin colour.

This takes between one and two years, depending on the location of the body being treated. However, in most cases the white spots reappear at the same location, often within just one year after stopping the treatments. This recurrence can be just as devastating as when the white patches first appeared.

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We wanted to find out why these spots reappear. Our research team suspected that “memory” forms within the skin when the white spots first appear, so that the spots “know” where to return when treatments are stopped. Working separately, we and three other laboratories led by Liv Eidsmo, Mary Jo Turk, and Julien Seneschal searched for the source of this memory in the skin.

These three other labs first found cells in vitiligo skin from mice or humans that looked a lot like the memory cells that protect the skin from a second exposure to a viral infection, suggesting that the body “thinks” it is fighting a viral infection when it “misfires” at the patient’s normal cells, killing the pigment-producing cells in the skin called melanocytes and causing vitiligo. These cells are called “resident memory T cells.”

Because immune resp**es to a virus act in a similar way to immune resp**es that cause autoimmune diseases, it seemed reasonable that these cells might also be the source of this remaining disease memory in the skin.

Disease memory can be erased with new treatment


We used a technique called skin blistering to isolate skin and skin fluid directly from the spots of my vitiligo patients and isolate the disease-causing memory cells so we could analyze them more closely. Similar to the other labs, we also found the virus-like memory cells, and we were able to also determine that these cells specifically targeted the melanocytes. We hypothesized that if we could remove these memory cells from the skin using a new treatment, then treatments to repigment the skin would be long-lasting and possibly permanent.

We then tested our hypothesis on mice we specifically engineered to develop vitiligo. Like humans, mice also have memory T-cells so we looked for their “Achilles heel” to see if we could knock them out without harming other cells. Our team figured out that the vitiligo-causing memory cells require a special protein called “IL-15” to survive. We injected the vitiligo mice with an antibody that blocks the IL-15 protein from interacting with the memory cells.

After just a few weeks we discovered that the treatment wiped out the memory cells from the mouse skin, allowing the brown pigment to return in a spotty pattern, just as we see in patients who respond to therapy. Importantly, just two weeks of antibody treatments caused repigmentation that lasted for months, suggesting this strategy, unlike existing treatments, might provide long-term benefit for vitiligo patients.

Human clinical trials may begin next summer


During our study we also found that the vitiligo-causing memory T-cells in both mouse and human skin seem to require IL-15 more than other types of T cells – which means they are more sensitive to levels of this protein. This is important because it means we might be able to selectively remove the vitiligo-causing cells without harming other important immune cells too. In the treated mice, the vitiligo-causing cells became undetectable, but the other T-cells resp**ible for fighting infection remained unharmed and present, suggesting that our antibody therapy might be safer for the immune system than first thought.

Based on these results, we are working with the National Institutes of Health-funded Immune Tolerance Network (ITN) to develop a clinical trial to test this antibody treatment in human patients. We are hopeful that we can begin recruiting patients next summer.

The ConversationAlthough this antibody drug has only been proven to work in mice with vitiligo, we are excited to test it in humans because it could represent a significant advance over existing treatments. The partnership with the ITN will allow us not only to test whether it works for vitiligo patients, but also how it works. This will help us know when and in whom to use this new therapy.

This article was originally published on The Conversation. Read the original article.

明年人身试验 呵呵
百度翻译下 很容易的

愿事如意

希望一切都是真的，希望胜利的日子早点到来！

123456dd

研究人员里面也有中国人

人工黑色素

我要报名当志愿者，冲我来

王雨雨

可不可以向冯某人求助，让他资助进行这项研究呢？造福人类造福下一代啊，朋友们发挥下才能吧！

李洋

这种研究的结果要么就收效甚微，要么就是特效治疗！

美丽的怅惘

还有很长的一段路要走！如果  真的需要资金  愿意奉献自己的力量！

锵锵

没看明白具体的治疗方法

色素丢失啊

感觉短期内是不会有新消息了，特效也很遥远

稻草人2018

我来大致总结一下：这位Harris教授发现白斑都会从同一个复发，有一定记忆效应，推测出白白不仅仅是免疫系统用T细胞杀死黑色素细胞造成的，而且会让T细胞长期驻守在白斑附近，被称为记忆T细胞。他们成功分离出这种细胞，发现这些记忆T细胞都需要一种特殊的L蛋白质，只要切断这种蛋白质的补充，记忆T细胞就会被杀死，黑色素细胞重新生长，白白会被根治。目前在老鼠身上有很好的效果。听着很有希望。