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輸入你的域名,以此为标准-yoursite.com

free website SEO report tooltips
← 點擊查看更新內容

中文网提醒: 请输入一级域名网址来索取中文报告,标准格式如 ‘yoursite.com’。
如果第一次系统不能快速生成报告,那是由于国内服务器速度快慢的原因,请刷新浏览器,重复一次就可以了。


網頁優化100分标准評級- determinedtosee.com

 網頁報告在生成當中 11月 24 2023 04:13 AM

舊的數據? {更新} !


你的網站分數是 47/100

emoji pink face 嵌入这个工具到你的网页!


Thank you dance animation
你的一个爱心分享,是我们生存下去的重要条件!


  過關,可以休息了

  還可以,建議繼續優化

  警告,建議修復

  錯誤,需要修復


搜索引擎报告100评分等级图表








  SEO內容  seo tooltips

標題  seo report title tooltips Determined to See

長度 : 17


accordion-arrow seo advice標題優化:


因为中文和英文的拼写不同,出现在谷歌搜索结果中的中文标题大概是30个文字,所以理想中文标题应该在25-30个文字之间。 網頁標題是搜索引擎檢索網頁排名很重要的一個元素,所以建議盡量優化長詞組的標題。


预览标题搜索语法:

在Google.com/baidu.com 上面输入 “site:yoursite.com” , 按回车健就可以查看了。你还可以查看到网页的收编数量。


   提示:SEO标题报告出现的警告和错误提示只针对于英文网站,中文网站可以忽视不理。


accordion-arrow 怎樣在你的網頁加入SEO標題標簽?


登錄到你的網站後台,找到要更新網頁的html代碼,搜索 < title > 標簽, 然後把網頁的標題寫到 < title > -- < /title > 中間。


如果你找不到 TITLE 標簽,那麼你就要自己把標題代碼寫進去, 不同的網站有不同的後台界面,你需要先找到網頁,然後再找要更新的代碼。


怎樣在 WORDPRESS 裏面撰寫標題代碼範例:
how to add webpage title tag

accordion-arrow 怎樣搜索盈利性的關鍵詞標題?



**几种搜索盈利性關鍵詞的方法


1. 使用 谷歌趨勢工具 來定位你的關鍵詞市場趨勢


2. 登錄谷歌廣告商ADWORDS帳號,使用谷歌關鍵詞工具來定位關於你生意的關鍵詞, 特點是多搜索量,少競爭,長詞組的關鍵詞。聯想用戶輸入關鍵詞的思路,撰寫用戶所需要的內容來解答他們的疑惑和需求。


谷歌關鍵詞工具預覽:
Google keywords planner tool


3. 在谷歌網站上面輸入關於你生意的關鍵詞,查看競爭對手在第一頁的排名,他們所使用的標題, 網頁的內容,思考你自己網頁所遺失的關鍵詞文章,然後重寫撰寫高質量內容的文章。 移動鼠標查看搜索結果的底部谷歌所建議關聯的關鍵詞,這些關鍵詞可能會幫助你的網頁增加曝光率和排名。


搜索結果底部谷歌所建議關聯的關鍵詞預覽:
google search result keywords suggests




4. 如果是搜索中文关键词组,建议可以用 百度指数 - 关键词工具



smiley face 關鍵詞詞組建議工具

accordion-arrow 預覽網頁標題源代碼



smiley face 預覽標題源代碼工具

描述

長度 : 0


accordion-arrow seo advice描述建議:


糟糕,我們沒有在你的網頁裏發現內容描述關鍵詞,它告訴搜索引擎有關於本網頁的內容。


在你的網頁最多可以寫上160個文字-描述標簽代碼,但是不能超過。它可以讓搜索引擎收編,告訴搜索引擎關於你網頁的內容大概。


怎樣撰寫網頁描述標簽代碼:

登錄到你的網站後台,找到要更新網頁的html代碼,搜索 <head> 標簽, 然後把網頁的描述META代碼寫到 <head> -- </head> 中間。


smiley face 生成 Meta Tags 代碼工具


accordion-arrowHTML5網頁SEO代碼結構範例如下:


** 不要拷貝 // 之後的內容, 它是為了解釋代碼如何使用。

如何使用代码?:拷贝这里的代码,修改成你自己网页的信息,然后到你的后台网页源代码,根据这个代码架构格式来进行黏贴。


<!DOCTYPE html> //定義HTML5文本樣式

<html lang="en-US"> //HTML5文本樣式顯示英文代碼

<html lang="zh-cn"> //HTML5文本樣式顯示中文代碼

<head> //HEAD標簽開始,在這裏面寫入的代碼不會顯示在網頁裏面

<meta charset="utf-8"> //UTF-8 代碼是為了顯示多語言文字

<meta name="viewport" content="width=device-width, initial-scale=1"> //手機屏幕伸縮顯示代碼

<link rel="canonical" href="https://www.metricbuz.com" /> // 告诉搜索引擎这个网页的优先权链接,注意链接要规范 + https:// 。

<title> 你的網頁主要標題寫在這裡 </title>

<meta name="keywords" content="寫入關鍵詞文字"> //網頁關鍵詞代碼

<meta name="description" content="寫入網頁描述"> //網頁描述代碼

<meta name="author" content="作者名字"> //作者名字代碼

<link rel=”author” href=”https://plus.google.com/+Metricbuzz-seo”/> // 使用 谷歌+ 语法在搜索结果中显示内容的原创作者。

<meta name="copyright" content="@All Rights Reserved"> //網頁版權代碼

<meta name="robots" content="index, follow"> //網頁蜘蛛收編文件代碼

<meta https-equiv="cache-control" content="cache"> //網頁缓存代碼,它加速你的網頁下載速度

<meta https-equiv="revisit-after" content="7 days"> //網頁重新訪問代碼,它告訴搜索引擎在7天後重新訪問檢索你的網頁

<meta https-equiv="refresh" content="30"> // 告诉搜索蜘蛛在30天之后执行更新内容检索命令。

<META NAME="ROBOTS" CONTENT="INDEX, NOFOLLOW">>
// 意思是搜索引擎蜘蛛检索这个网页, NOFOLLOW 就是不让这个网页里面的外链在搜索引擎产品价值。 举例:假设你的网页链接出现在某个网页,但是这个网页设置了 NOFOLLOW 指令, 那么你的这个网页链接就不再在搜索引擎的排名结果中产生价值。



下面5行是社交网站的代码

<meta property="og:title" content="这里输入标题"> // 告诉脸书你的网页标题
<meta property="og:description" content="这里输入描述"> // 告诉脸书你的网页描述内容
<meta property="og:type" content="这里输入内容模式"> // 告诉脸书你的网页内容
<meta property="og:image" content="https://example.com/image.jpg"> // 告诉脸书你的网页图片
<meta property="og:url" content="https://www.example.com/"> // 告诉脸书你的网页链接



下面5行是分享到 TWITTER 上面的内容代码

<meta name=”twitter:card” content=”summary”> // 告诉推特你的网页内容总结

<meta name=”twitter:url” content=”https://www.metricbuzz.com”> // 告诉推特你的网页链接

<meta name=”twitter:title" content=”这里输入标题”> // 告诉推特你的网页标题

<meta name=”twitter:description” content=”这里输入描述”>
// 告诉推特你的网页描述

<meta name=”twitter:image” content=”https://www.metricbuzz.com/metric-buzz-logo.png”> // 告诉推特你的网页图片



</head> //HEAD標簽結束

<body> //在 body標簽 裏面寫入的代碼會顯示在網頁上面

<h1>這裡寫入內容 </h1> //H1 到 H6 的文字標簽代碼,顯示文字的大小

<h2>This is a Heading </h2>

<h3>This is a Heading </h3>

<h4>This is a Heading </h4>

<h5>This is a Heading </h5>

<h6>This is a Heading </h6>

<p>這裡寫入段落內容 </p> //普通文字段落標簽代碼

<img src="example.img" alt="在這裡寫入圖片的名字"> //圖片標簽代碼

<iframe src="https://www.metricbuzz.com">
<p> 你的瀏覽器不支持內置窗口 </p>
</iframe> //Iframe 內置窗口表示在同一個網頁,有另外一個窗口,它是不好的搜索引擎操作。



下面是 ’架构数据代码‘, 它告诉搜索引擎关于你的各类商业信息,增加你的商业网上曝光率。

架构数据代码生成工具

<div itemscope itemtype="https://schema.org/LocalBusiness">
<span itemprop="name">Search Buzz Inc</span>
<div itemprop="address" itemscope itemtype="https://schema.org/PostalAddress">
<span itemprop="streetAddress">1000 main st</span>
<span itemprop="addressLocality">Flushing</span>,
<span itemprop="addressRegion">NY</span>
<span itemprop="postalCode">11354</span>
</div>
Phone: <span itemprop="telephone">9173304930</span>
<a href="https://www.google.com/maps/place/1000+Main+St,+Flushing,+NY+11367/data=!4m2!3m1!1s0x89c2608d1d514f07:0x663177ad64962765?sa=X&ei=Q6qDVeKkI4L6sAW5_YPABw&ved=0CB0Q8gEwAA" itemprop="maps">URL of Map</a>
</div>



</body> //BODY 標簽結束

</html> //整個網頁文本代碼結束

關鍵詞  seo report keywords tooltips





开放圖形元素协议









accordion-arrow seo advice優化建議:


糟糕,此頁面不包含 “Og Meta Properties” 標簽,這個標籤允許社交網站爬蟲更好的理解你的網頁內容。 此標簽代表一種 “开放圖形元素协议”,可以在你的網頁頭部代碼嵌入此標簽,詳見下面的代碼例子:


"Og Meta Properties" 是社交網站使用的標簽代碼


查看以下範例:

<meta property="og:title" content="這裡輸入標題內容">
<meta property="og:description" content="這裡輸入描述內容">
<meta property="og:type" content="article">
<meta property="og:image" content="https://example.com/image.jpg">
<meta property="og:url" content="https://www.example.com/">

smiley face

使用 Og Properties 代码自动生成工具

了解更多社交網代碼知識

登录你的脸书账号来查看你的网页OG社交代码是怎么工作的?

頭條
H1 H2 H3 H4 H5 H6
0 19 4 1 0 0
  • [H2] Determined to See
  • [H2] Survey Shows Curcumin, Black Pepper, Ginger Combo Improves RP Vision
  • [H2] How’s Your Self Compassion and Love?
  • [H2] Focus Now Available as an Audiobook
  • [H2] Late Stage RP Sufferer Yields Ongoing Vision Gains with Curcumin, Black Pepper and Ginger
  • [H2] Nanoscope Wins Breakout Technology Award for Vision-Restoring Drug
  • [H2] Drug to Treat Alcoholism Restores Vision in Mice with RP
  • [H2] Practicing Gratitude and Giving the Budwig Protocol a Try
  • [H2] Making a Miracle: The Decades-Long Journey Behind Nanoscope’s Vision-Restoring Drug
  • [H2] The Backstory
  • [H2] The Breakthrough
  • [H2] Next Steps
  • [H2] Nanoscope Therapeutics Restores Meaningful Vision with Universal Optogenetics Therapy for Late Stage RP
  • [H2] Chemically Induced Retinal Cells Offer Vision Restoration Hope for RP
  • [H2] Newsletter
  • [H2] Join the Conversation
  • [H2] About the Blog
  • [H2] Subscribe to Blog
  • [H2] Recent Posts
  • [H3]
  • [H3] The Backstory
  • [H3]
  • [H3] Next Steps
  • [H4] I SPICE NEWSLETTER #12




圖片 我們在當前網頁檢索到 118 個圖片。



accordion-arrow seo advice優化建議:


糟糕,10 個圖片ALT屬性是空的,或者丟失。添加ALT屬性,以方便搜索引擎可以更好地了解你的圖片內容。


怎樣撰寫圖片 Alt 屬性範例:

<img src="example.img" alt="寫入圖片的有關內容描述" width="300" height="200">,准确描述图片的大小/width/height可以让网页下载的更快。


如果谷歌网页速度工具 给予你的网站低的速度评分,最快的方法就是优化你的图片, 然后再查看一下你的网页速度,你会发现分数很快提高了不少。

如果你使用https,而不是https, 请务必检查你的图片链接。

使用 图片优化工具.



smiley face 寻找物廉价美的平面设计图片服务


free vector 超过600,000免费+付费网页设计图片下载

文本/代碼 比例  seo report Text HTML Ratio tooltips 比例 : 0%









accordion-arrow seo advice內容優化建議:


糟糕,當前網頁 文本/HTML 代碼的比例低於15%, 這意味著你的網頁可能需要更多的關鍵詞文字內容。


accordion-arrow基本撰寫網頁內容策略



撰寫網頁有效內容策略應該是對搜索引擎來說最重要的事情了。它讓搜索引擎不斷收編你的網頁鏈接,內容,增加搜索結果,潛在流量。 有效的網頁內容也大大提高了用戶的滿意度,解答用戶潛在的各種問題,不斷增加潛在成交量。 所以,在撰寫內容之前,必須深思熟慮,先問自己下面的幾個問題?


  • 誰是你的潛在用戶,你了解他們的需求嗎?如果答案不是,你應該先要進行有效的市場調研,學習潛在用戶行為,然後再來撰寫針對性的網頁內容。

  • 在不斷了解潛在用戶的思維方式和行為之後,你應該不斷換位思考,從用戶角度需求出發,撰寫他們所需要的內容。

  • 你應該設計一個用戶體驗良好的網站,比如容易瀏覽,快速簡易查找相關信息,可讀性, 不應該讓用戶思考怎樣使用你的網站,還有,不要讓他們在使用網站的過程中填寫很多不必要的信息。

  • 網站可用性意味這:快速的網頁,手機屏幕伸縮設計,愉悅的可讀性文字, 連貫的的設計顏色。 設計信息图表內容是一種很好的方式來同你的用戶分享信息,研究報告人的大腦更容易記住關於圖片的信息。

  • 始終思考怎樣病毒式的传播你的內容。你可以設計視頻內容來推廣你的生意,你可以在你的網站提供免費的工具代碼給別人用,然後再鏈接到你的網頁去。 你還可以設計相關的遊戲內容,打遊戲競爭級別是人的天性,有利於傳播你的網站。 如果你撰寫的文字內容非常有用,可以解決別人的實際問題,這也可能產生被傳播的機率。

  • 除了上面的,始終撰寫你自己熟悉的內容主題是非常重要的。



smiley face 查看潛在錯誤英文語法,抄袭内容工具
動畫



accordion-arrow seo advice優化建議:


完美,在這個頁面上沒有檢測到 Flash 動畫內容。


Flash 動畫 HTML 代碼:

<body>
<object width="400" height="400" data="helloworld.swf"> </object>
</body>

smiley face 動畫範例網頁:
浮動框架





accordion-arrow seo advice優化建議:


不錯! 在這個頁面上沒有檢測到內部框架,Iframe 就是在網頁中有一個小的滾動窗口,這可能導致搜索引擎很難索引到網頁內容。


內置窗口 HTML 代碼:

<iframe src="https://www.metricbuzz.com">
<p> 你的瀏覽器不支持內置窗口 </p>
</iframe>

smiley face 查看內置窗口範例:

  SEO鏈接  seo report SEO links tooltips

獨立鏈接重寫







accordion-arrow seo advice優化建議:


不錯,你的網頁鏈接看起來友好,包含關鍵詞!


如果你想要重新編寫網頁包含關鍵詞的鏈接,把下劃線 _ 改稱- 的話, 你需要修改一個服務器根目錄 public_html 下面的文件名 ".htaccess"。


鏈接重寫範例:

不友好的鏈接:

https://www.example.com/seo*%&^links.html
(鏈接有許多搜索引擎不理解的符號 *%&^ )

重寫後的鏈接範例:

https://www.example.com/seo-links.html
下劃線的獨立鏈接









accordion-arrow seo advice優化建議:


糟糕!在您的網址鏈接檢測到下劃線 _,你應該用連字符 - 來優化你的SEO鏈接,搜索引擎更加理解 - 的鏈接。


鏈接不友好範例:

https://www.example.com/seo_links.html

鏈接友好範例:

https://www.example.com/seo-links.html

如果你想要重新編寫網頁包含關鍵詞的鏈接,把下劃線 _ 改稱- 的話, 你需要修改一個服務器根目錄 public_html 下面的文件名 ".htaccess"。

我們對當前網頁檢索到了 50鏈接

關鍵詞鏈接 鏈接類型 鏈接價值
- 內部鏈接 傳遞價值
Home 內部鏈接 傳遞價值
About Ingrid 內部鏈接 傳遞價值
My Books 內部鏈接 傳遞價值
About Jeanne 內部鏈接 傳遞價值
My Art: Eye Will Artistry 內部鏈接 傳遞價值
About Retinitis Pigmentosa 內部鏈接 傳遞價值
RP Acupuncturists 內部鏈接 傳遞價值
Survey Shows Curcumin, Black Pepper, Ginger Combo Improves RP Vision 內部鏈接 傳遞價值
Uncategorized 內部鏈接 傳遞價值
1 Comment » 內部鏈接 傳遞價值
How’s Your Self Compassion and Love? 內部鏈接 傳遞價值
6 Comments » 內部鏈接 傳遞價值
Focus Now Available as an Audiobook 內部鏈接 傳遞價值
click here 外部鏈接 傳遞價值
No Comments » 內部鏈接 傳遞價值
Late Stage RP Sufferer Yields Ongoing Vision Gains with Curcumin, Black Pepper and Ginger 內部鏈接 傳遞價值
click here 外部鏈接 傳遞價值
click here 外部鏈接 傳遞價值
4 Comments » 內部鏈接 傳遞價值
Nanoscope Wins Breakout Technology Award for Vision-Restoring Drug 內部鏈接 傳遞價值
Nanoscope Therapeutics 外部鏈接 傳遞價值
click here 內部鏈接 傳遞價值
click here 內部鏈接 傳遞價值
1 Comment » 內部鏈接 傳遞價值
Drug to Treat Alcoholism Restores Vision in Mice with RP 內部鏈接 傳遞價值
Berkeley News 外部鏈接 傳遞價值
Science Advances Journal 外部鏈接 傳遞價值
2 Comments » 內部鏈接 傳遞價值
Practicing Gratitude and Giving the Budwig Protocol a Try 內部鏈接 傳遞價值
2 Comments » 內部鏈接 傳遞價值
3 Comments » 內部鏈接 傳遞價值
Nanoscope Therapeutics, 外部鏈接 傳遞價值
clinicaltrials.gov 外部鏈接 傳遞價值
25 Comments » 內部鏈接 傳遞價值
Chemically Induced Retinal Cells Offer Vision Restoration Hope for RP 內部鏈接 傳遞價值
CiRC Biosciences 外部鏈接 傳遞價值
Paragon 外部鏈接 傳遞價值
Ingrid Ricks 內部鏈接 傳遞價值
Retinitis Pigmentosa 內部鏈接 傳遞價值
Reversing Blindness 內部鏈接 傳遞價值
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Vision Restoration 內部鏈接 傳遞價值
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adazing web design 外部鏈接 傳遞價值




  SEO 關鍵詞

關鍵詞雲 address see determined email
連貫性關鍵詞
關鍵字 內容 標題 關鍵詞 描述 頭條
determined 1
see 1
email 1
address 1



accordion-arrow seo advice優化建議:


對於搜索引擎來說,最好的策略是不斷地撰寫有效地內容來提高網頁在搜索引擎地排名和瀏覽。


基本撰寫網頁內容策略


smiley face 查看關鍵詞密度工具
smiley face 使用 谷歌站长工具 来了解用户搜索关键词行为?

smiley face 使用 谷歌网站分析工具 来查看网站关键词报告?

安装好谷歌网站分析工具后,你可以登录到后台,设置让这个工具每个礼拜给你GMAIL发网站报告邮件,请看下面截图范例。


查看关键词难易排名工具 查看整个网站后缀链接魔法工具


  可用性建議  seo report Usability tooltips

獨立域名鏈接 域名 : determinedtosee.com
長度 : 19






seo advice優化建議:

accordion-arrow域名可用性建議 & 各類工具:


通常情況下,你的域名越短越好,6-7字母(不包括.com)是比較理想的域名。 域名的名字應該讓用戶很容易的記住,並且經常回來瀏覽你的網頁。


如果你的域名太長了,用戶就不容易記住,那訪問的機會就會大大降低。 你的域名應該俱有創意,和你的生意內容相關,可以讓用戶需要服務的時候聯想到你的生意,這對於生意長久的營銷非常有利。



smiley face

網站速度測試工具

網上聲譽檢查工具

網站病毒檢查工具

** 使用以下的搜索引擎蜘蛛爬行文件工具來生成代碼,文件名為 "robots.txt", 然後上傳文件名到服務器上面去,目錄路徑為 "public_html/robots.txt".

生成搜索引擎蜘蛛爬行文件工具

robots.txt 文件網頁範例


** 查看每個網頁的內存大小,建議不要超過100K,如果一個網頁的內存太大,那麼網頁的下載速度就會降低,影響用戶體驗。

查看網頁內存大小工具 check webpage size
網頁頂部小圖標








accordion-arrow seo advice優化建議:


不錯,你的網站發現 favicon快捷方式圖標,它在網站瀏覽器 頂部窗口最左邊。


** Favicon 文件名為 "favicon.ico",尺寸為 50X50 pixels/皮克, 生成好這個小圖標之後,上傳到服務器的根目錄,為 "public_html/favicon.ico"。


smiley face 小圖標生成工具

網站小圖標範例:
metric buzz favicon

可打印的





語言



accordion-arrow seo advice優化建議:


不錯,當前網頁發現語言代碼標簽--/html lang="en-US"/。


網頁語言代碼英文標簽範例: <html lang="en-US">

網頁語言代碼中文標簽範例: <html lang="zh-cn">

元数据元素集合








accordion-arrow seo advice優化建議:


糟糕,當前網頁沒有使用 Dublin Core 代碼標簽(Dublin Core 是由15個資源描述代碼標簽組成的詞彙)。


查看 Dublin 代碼標簽 如下範例:

<metadata xmlns:xsi="https://www.w3.org/2001/XMLSchema-instance">
<meta name="DC.title" content=" 你的網頁主要標題寫在這裡 " />
<meta name="DC.Creator" content=" 作者名字寫在這裡 " />
<meta name="DC.subject" content=" 網站主題寫在這裡 " />
<meta name="DC.description" content=" 你的網頁描述寫在這裡" />
<meta name="DC.publisher" content=" 你的公司名字寫在這裡 " />
<meta name="DC.date" content=" 2014-12-01 " />
<meta name="DC.type" content=" 網站大概內容寫在這裡 " />
<meta name="DC.language" content=" en-US " />
</metadata>

smiley face Dublin Core 代碼生成工具





  網頁文本  seo report Document tooltips

文檔類型 XHTML 1.0 Transitional
robots.txt tooltips
Yoursite.com/Robots.txt 文件 Determined to See

Determined to See

Survey Shows Curcumin, Black Pepper, Ginger Combo Improves RP Vision

Written By: ingridricks - Dec• 12•22

For those of you who missed this story, Steve Fialkoff, a 68-year-old New Yorker with the Usher 2A RP mutation, stumbled on a combo of curcumin, black pepper and ginger last February that started giving him back bits of eyesight.

Determined to spread the word about his discovery, the video-editor-turned-playwright who should also consider a career as a comedian, reported his vision gains to a retinal specialist, who immediately dismissed his curcumin, black pepper & ginger claims. Undeterred by her lack of enthusiasm, he shared his news with Foundation Fighting Blindness, and was told that extensive research would be required to determined if his experience with curcumin and ginger was more than a fluke. So Steve took what he saw as the only logical next step: launching his own, informal Curcumin RP study – which he named I SPICE (Improving Sight Project Investigating Curcumin Experiment).

Steve’s ever-growing I SPICE group currently consists of 56 RP participants who are all experimenting with different combos of curcumin, black pepper and ginger. And the first survey results – tallied over Thanksgiving weekend – indicate that curcumin with ginger does indeed improve RP eyesight.

Of the thirty participants who took part in the survey, fifteen reported vision improvements. Some report expanded visual fields. Others have seen a jump in visual acuity and color. A couple have even received a boost in their night vision. Not everyone has experienced vision gains. My curcumin experiment has so far only yielded occasional, inconsistent increases in visual acuity. But I am excited about the results because they span several RP mutations — something that has now caught the attention of FFB. According to Steve, the foundation is now considering a curcumin RP study. In the meantime, Steve is tracking a curcumin macular degeneration study being conducted by the University of Illinois. Based on the positive results of a research study utilizing the amino acid N-Acetyl Cysteine (NAC) for RP treatment, some of us I SPICE participants are also starting to add it into the experiment mix.

It’s been so empowering to be on this journey with Steve and the other RP participants and if you are interested, we would love to have you join. The more data we can collect and information we can share – the closer we all are to seeing our world. To join the I SPICE experiment, email Steve at: [email protected].

And to get a sense for Steve and the amazing work he is doing on our behalf, check out his December 8 e-bulletin, which I’ve pasted below.

I SPICE NEWSLETTER #12

Dec. 8, 2022

Improving Sight Project 

Investigating Curcumin Experiment

Topics:

1) New reports

2) FFB on the case

3) New experimenters

1) New Reports:

A recent Curcumin experimenter with 99% vision loss with a recessive FAM gene type reports her latest doctor eye exam from Wills eye institute.

Her last check was two years ago.

She saw the first two lines of the Snellen chart. Big E, and the next line. She was told she had 20-400 vision. Also, she scored correctly on identifying black and white squares with her bad eye. Ok, so? It doesn’t sound so great. Well, she didn’t have any vision to measure two years ago. What was the eye doctor’s response to this test finding?:

“You must have had a bad day two years ago. I doubt Curcumin is responsible for these test results…”

To quote my own dialogue line from a play I wrote:

“Doctors Schmocktors!”

The same woman reports visiting her friend and seeing her new bangs on her forehead when she turned her head into he sunbeam coming in from the window.

What I love about this report is the modesty and uncertainty about her own improvement.

“Maybe it’s my imagination and I could see this stuff all along but just now hyper aware of any object in view” She told me over the phone.

Ok, let’s give it another month and see what happens.

She is also starting to take N-Acetyl Cysteine.

Which leads us to a second report from Me.

I haven’t noticed any big improvements since October, ’22.

But after having, coincidentally, blended ginger strips in my lentil soup, my left eye seems to be seeing more, enabling it to lock with my right eye for longer periods of time especially in daylight when there is more light out there. Less double vision means a wider tunnel to view the world through. I also take 1 gram of N-Acetyl Cysteine a day along with the Curcumin. (I don’t know if NAC increases anti-coagulation but I will check on that.) The NAC is about a month into my regimen.

Ok, it’s only been 3 days of this increased field but it is strange that it happened after eating ginger in lentil soup meal.

(yes, there was black pepper, garlic, olive oil, butter, salt, shallots in the flavorings well)

Was it good? 

Eh, it was very hearty.

Does it make a lot of gas?

NAC + lentils = gas

NAC + anything= gas

2) FFB on the case:

The word from the FFB is encouraging. Since twenty more people could have potentially reported but didn’t… our data sample was relatively tiny.

Very hard to spot a pattern or trend in such little data.

But, I believe the data shows that Curcumin doesn’t care which gene you have mutated. Recessive forms may respond better. USH2A seems to respond favorably. (I have that one, which is supposed to be the most common form of RP)

Too early to tell is the word but I believe that Autosomal dominant P23 H rhodopsin type isn’t the only RP to benefit from a possible Curcumin therapy.

All in all the fact that 15 out of 30 reports were positive improvement, is pretty compelling info.

Additionally,

I am awaiting safety and efficacy results from Univ. of Illinois at Chicago trial of curcumin on Macular degeneration.

I believe, if no adverse effects are found, then creating a human trial with curcumin and RP will be a no brainer.

We shall see.

3) New experimenters:

There are two new experimenters as of last week. The word is spreading albeit, slowly. Both of them have Ushers with hearing loss and RP.

Will Curcumin help hearing and seeing? Perhaps we can help two verbs with one pill?

Oh, that was terrible, steve!

Anyway, I hope to be hearing from people who just started at the end of October.

Keep in touch.

Avoid the flu.

Curcumin is derived mostly from turmeric root a member of the ginger family, which includes Black pepper. 

I use fresh ground black peppercorns, fresh sliced and peeled ginger root cooked in olive oil or butter or ghee or coconut oil.

My calculations show 1/5 of a teaspoon of ground black pepper supposedly contains enough Piperine to activate curcumin in the blood stream.

Or just take it in your favorite brand’s capsule. I don’t have an amount for ginger either. I just use a coin sized slice per day, after it’s been cooked.

I don’t know if sugared and brined ginger from the Sushi bar works. I also cannot say that it doesn’t work either.

Nobody said this was going to be easy.

Disclaimers:

Steve NYC

1- there is no proof in the literature that Curcumin will help humans with RP.

2- there are no human safety trials for RP people using Curcumin supplements

3- I am not a doctor

4- Curcumin at certain levels may interact with other medications you may be taking.  Large amounts may cause bleeding. Consult a doctor.

5- I do not know what these levels are.

6- Consult a medical professional before starting on any therapy

7- According to the Italian researchers in the May 2021 review article linked below, there are some forms of RP that will not respond to Curcumin

8- Short term risks or benefits have not been established.

9- This is information and not medical advice.

10- I suggest you read the research on the NIH.gov site.

11- I do not sell Curcumin or NAC or work for any company that makes any supplement product. Therefore I do not have any monetary compensation from the sale of this substance.

12- I’m just a guy with RP for sixty-eight years.

https://www.dovepress.com/recent-advances-and-disputes-about-curcumin-in-retinal-diseases-peer-reviewed-fulltext-article-OPTH

The end.

Join the conversation!

How’s Your Self Compassion and Love?

Written By: ingridricks - Oct• 07•22

It hit me last night that I’ve done a really lousy job of this. I’ve been so focused on putting on a cheery face and a positive all-is-great attitude so that the Universe will deem me worthy of getting back my eyesight that I punish myself every time I make a misstep.

If I feel sad it means I’m focusing on my loss and drawing negative energy my way. If desperation sometimes overtakes me, it means that I’m not trusting and allowing that it’s out there for me. If I take a day off from staring into a color therapy lamp, applying micro current stimulation to my eyes and doing deep breathing to increase blood flow and circulation to my eyes along with every other thing I try, it means I’m not doing what it takes to earn back my vision. If I don’t accept my current lack of eyesight while I hold on to hope that an answer will soon materialize, it means I’m making my life harder for those I love. 

As I laid in bed last night pummeling myself for having all of these emotions, I realized I needed to take a step back and just love myself — and give myself some grace for being human.

I think it’s human nature to stuff down grief and trauma and charge forward with our lives, believing that if we give into the feelings it means we are somehow weak or not resilient. But I’ve realized that this approach can be really harmful. 

So I’m setting out on a new quest today. I’m really going to focus on self compassion and love. I’m going to be kind to myself when these emotions bubble up and trust that the Universe has my back anyway. My first step in self love is to admit that I have these emotions and that it’s okay. And tonight, instead of immersing myself in another self-help book in search of an answer, I’m going to settle into my hot tub with a full glass of wine and Billie Holiday singing away — and afterward, I might even indulge in some dark chocolate.

Okay — now it’s your turn. How are you showing yourself some compassion and love? Please let me know so I can share it here. And in the meantime, know that I am sending lots of love your way.

Join the conversation!

Focus Now Available as an Audiobook

Written By: ingridricks - Sep• 14•22

My memoir about my early journey with RP is finally available as an audiobook and I was given 25 free promo codes for anyone who is interested.

I wanted to share it here because I know my journey will resonate with a lot of you. My next book is going to end with me getting my eyesight back. 🙂

Below is more info on the book. If you are interested in listening to it and would like the promo code, click here.

From the Author of the New York Times bestseller Hippie Boy: A Girl’s Story

At the age of 37, Ingrid Ricks learned she suffered from Retinitis Pigmentosa, an incurable eye disease that was stealing her eyesight and would eventually leave her completely blind. Gripped with the terrifying fear that she would miss out on her daughters’ lives, become a burden to her husband, and lose the career and independence that defined her, Ingrid embarks on a quest to fix her eyesight that ends up fixing her life. 

Join the conversation!

Late Stage RP Sufferer Yields Ongoing Vision Gains with Curcumin, Black Pepper and Ginger

Written By: ingridricks - Sep• 01•22

Steve Fialkoff was only trying to boost his immune system when he started ingesting 250 milligrams of curcumin daily last December. The sixty-eight-year-old New Yorker had contracted Covid-19 and hoped the plant-based supplement — which is known for it’s anti-inflammatory and antioxidant properties — would help combat the virus. 

He didn’t give it much thought until February 8th, when he was out walking his guide dog. Usually Steve could see half of his dog’s head, one of his eyes or his tail wagging in a blurry narrow tunnel. But that morning, when he looked at his dog, Steve says he could see his entire head, whole body, individual hairs standing up and his tail all in one glance.

“Then I looked down on the sidewalk and realized that I could see the side of an apartment building and cars parked on the curb,” Steve adds. “In December, or even a week earlier, I wouldn’t even have been able to tell where I was because my vision was so narrow.”

Steve, a two-time Emmy-winning video editor who was forced to leave his career when his vision closed in on him, was convinced he was hallucinating. But when he returned to his Manhattan apartment and walked into his kitchen, he noticed that instead of seeing only one burner on his four-burner stove, he could see three and a half. And the only thing he could conclude is that his sudden jump in vision was connected to the curcumin he was taking.

His daughter did a Google search for the key words curcumin and Retinitis Pigmentosa and was immediately directed to a May 2021 research paper in which Italian researchers compiled all the studies done to date on curcumin and its positive impact on retinal diseases.

“The 30-page document talked about a study in which curcumin was fed to rats with RP and theorized that it would take a dose of three or four grams in people with RP to achieve the benefits,” notes Steve. “That’s a mistake because I was only taking 250 milligrams.”

In closer inspection of the label on his curcumin supplements, Steve discovered that it recommended 500 milligrams daily so he started taking it more religiously and upping the dose. On March 11th, Steve experienced another jump in vision. This time, he says he could see leaves on trees and people walking toward him.

Steve racked his brain, trying to figure out what else he was doing that could account for his vision gains. Once again, he pulled up the 30-page article on curcumin and retinal diseases. But this time, he decided to comb through it carefully in its entirety. Most of it, says Steve, was “garbley-gook”. But then he got to the end of it and discovered that the key to activating curcumin is piperine, the active ingredient in black pepper. According to the article, twenty milligrams of piperine increased curcumin absorption by two-thousand percent. Steve also discovered that it took about forty-eight hours for the curcumin to get into the retina after ingesting the two.

He started thinking about the ginger chicken he had ordered from his favorite Vietnamese restaurant three days earlier. It was a dish that contained an extensive amount of black pepper.

“I had my daughter check my credit card receipts and discovered that the last time I had ordered that dish was on February 4, a few days before my first jump in vision. I thought, aha, here it is. I accidentally took curcumin and accidentally took black pepper and it’s generating vision gains.”

Steve, who has the Usher 2a form of RP, was so excited by his discovery that in April he reported his vision gains to his retinal specialist. She conducted a visual acuity test and discovered that the vision in his right eye had increased from 20/400 to 20/250. Beyond that, Steve estimates that his central visual field has expanded to about six degrees, a big jump from the narrow two-degree hole he had been seeing out of. Because eye doctors had stopped measuring his visual field a decade ago, there was no way to measure that expansion during his visit. What’s more, Steve says his retinal specialist wasn’t interested when he told her his vision jump was due to curcumin.

Steve, who had heard about other treatments such as acupuncture and Chinese herbs that had helped RP sufferers for a month or two but then stopped working, sometimes had doubts and waited for the other shoe to drop. But he kept adding black pepper to his meals and kept taking the curcumin and his vision gains held steady. In July, he decided to look up the recipe for the ginger chicken dish that had precipitated both jumps in vision. That’s when he discovered that a heavy dose of black pepper was sautéed in oil with ginger for several hours. In further research, he learned that heat and fat also help with activation and absorption of curcumin, and that ginger is also beneficial for the retina. Steve began replicating the recipe at home and, two weeks later, he experienced another jump in vision. This time, he noticed that he could see when walking through a scaffolding tunnel where the light was lower, something he hadn’t been able to do for several years. He also noticed that he could see more detail in bright light.

He decided it was time to call the Foundation Fighting Blindness to share his vision gains with curcumin. He was routed to their science reporter, who noted that an Indian researcher they fund had identified curcumin as having a positive effect on a rare form of RP. But he also said they would need more double-blind studies to confirm this finding.

“I wasn’t going to argue with this guy,” notes Steve. “I didn’t want to sound like a petulant brat. But I know in my heart we don’t need a double-blind study. We need a study, with twenty or thirty people, and if they don’t go blind and some of them get better, then something is happening.”

This is where Steve comes in. He has launched his own informal curcumin experiment and currently has twenty people — most with RP and a few with other retinal diseases — on board. Not everyone is following his regimen. Some are ingesting piperine supplements with curcumin supplements. Others are experimenting with whole turmeric — the plant responsible for curcumin. Still others are mixing both turmeric and ginger. Steve will be sharing the results as they come in.

He doesn’t know if his curcumin concoction works for every form of RP or whether his eyesight will continue to improve. But for him, the vision gains he has experienced over the past eight months are nothing short of miraculous.

“In a way, it’s a good thing that I was almost blind. Because if my visual field was 15 or 20 degrees and I still had good central vision, I probably wouldn’t have noticed the vision gains and would have eventually stopped taking curcumin,” notes Steve. “Before, I would say that I was 98 percent blind. Now I estimate that I am 93 percent blind and back to the vision I had in 2018. I’m just going to keep going and see what happens.”

If you would like to join Steve’s curcumin experiment, please email him at: [email protected]

To read the May 2021 article on curcumin and retinal diseases, click here.

To read the January 2022 article on curcumin and retinal diseases, click here.

Join the conversation!

Nanoscope Wins Breakout Technology Award for Vision-Restoring Drug

Written By: ingridricks - Jul• 24•22

Nanoscope Therapeutics was recently singled out for its ground-breaking optogenetics drug at the OIS Retina Innovation Summit in New York, the latest achievement in the company’s quest to restore meaningful vision to the millions of us suffering from debilitating retinal diseases.

Since announcing the remarkable results of its Phase 1/2a clinical trial for Retinitis Pigmentosa last June, the company has been on a tear — launching a Phase 2b clinical trial for RP as well as a Phase 2 clinical trial for Stargardt disease. Results from both of these trials will be announced first quarter of 2023. I have been watching Nanoscope closely over the past year because as far as I can tell, it offers the best hope for vision restoration in those of us living with late-stage RP — regardless of gene mutation. I had the opportunity to interview both CEO, Sulagna Bhattacharya, and President, Samarendra Mohanty, and was moved by their incredible passion and commitment, which at this point has been decades in the making.

To read more about Nanoscope’s remarkable results in their Phase 1/2a trial in India, click here.

For a deep dive into the decades-long journey behind this game-changing drug, click here.

Join the conversation!

Drug to Treat Alcoholism Restores Vision in Mice with RP

Written By: ingridricks - Mar• 29•22

Researchers at University of California, Berkeley and UC Santa Barbara have discovered that disulfiram, a drug that combats alcoholism, may also be the key to restoring vision in people with advanced RP and age-related macular degeneration.

The key is that disulfiram, which inhibits enzymes involved in the body’s ability to degrade alcohol, also impedes the enzymes that make retinoic acid. What makes this so critical is that researchers have found that retinoic acid interferes with light perception in those with RP. By inhibiting the enzyme that creates reitinoic acid, they were able to eliminate the interference in nearly blind mice, enabling them to see images on a computer screen.

I’ve reached out to the researchers involved in this trial for an interview but have not yet heard back from them. However, here is the gist:

  • Disulfiram has already been approved by the FDA for treatment of alcoholism — which greatly reduces the barriers for making disulfiram available as a treatment for people suffering from RP.
  • The drug has very little known side-affects, unless you drink alcohol — in which case, it will make you relive your worst hangover (think severe vomiting, headache, etc.).
  • The next step, according to news reports, is a clinical trial in which researchers will team with a handful of ophthalmologists to administer the drug to patients with advanced RP (but not complete retinal degeneration).

Here’s a link to a detailed article that appeared in Berkeley News and here’s a link to the Science Advances Journal article.

Bottom line — great news.

Join the conversation!

Practicing Gratitude and Giving the Budwig Protocol a Try

Written By: ingridricks - Jan• 07•22

I didn’t think doctors or researchers would ever crack the code to my RP-suspected vision loss. I don’t have any family history and the two genetic tests I underwent in 2018 came up empty. But with all the breakthrough medical advancements now being made on the RP front, that might as well have been light years ago. 

In the last three years alone, researchers have identified 140 new gene mutations associated with RP, bringing the total to around 320. So, at the urging of a new retinal specialist, I gave it another go. And lo and behold, eight gene mutations linked to RP were found. At first, I didn’t understand why knowing these mutations were of benefit to me because it’s not like I have a strong dominant gene that is being targeted for gene therapy. But as it turns out, having a known gene association with RP is a key criterion to participate in any of the promising RP clinical trials underway — including the gene agnostic optogenetics therapy developed by Nanoscope therapeutics now being tested in a phase 2B clinical trial throughout the US.

Beyond this, in my case, I’ve uncovered a critical clue that may be tied to both my vision loss and the triple-negative breast cancer I was diagnosed with six years ago: Arginine, an essential amino acid that is critical for blood flow and circulation, is being stripped from one of my genes.

This was a light bulb moment for me and has led me to adopt the Budwig protocol, which was developed by German Biochemist Johanna Budwig to treat cancer patients. What she discovered is that, like me, severely ill cancer patients were missing this essential amino acid in their cells. It’s a key ingredient in flaxseed oil. The problem, according to Budwig, was that in order for cells to absorb this essential amino acid, the oil needed to be delivered through a water-soluble mechanism. To solve this issue, she blended flaxseed oil with low-fat cottage cheese (or quark), which makes the oil water-soluble.

There is limited research on the Budwig Protocol, though many cancer survivors swear by it. And given that this essential amino acid is also critical to eye health, Budwig Protocol here I come. 

What I know for certain is that vision-restoring answers are finally on the way for us. In the meantime, we have got to do our part. We have to do everything we can to slow the degeneration so our retinas are in the best shape possible for the emerging therapies. Knowledge is power, so the more we learn about our specific mutations through the extensive genetic testing now available, the more we help researchers help us — and the more we may be able to help ourselves.

Because of my recent genetic test results, I have a new tool I can add to my personal eyesight retention and restoration plan. And that, along with the regular OTC scans I’m now undergoing to carefully track and monitor my retina and any changes occurring, ensures I can be ready to jump as soon as the right therapy for me materializes.

I’m shouting out my gratitude to every researcher, scientist, and eye doctor who are working on our behalf — as well as to the many foundations and individuals who have and continue to generously fund eye research. Thanks to all of you, I know I’m going to see my family’s faces and my world again.

Join the conversation!

Making a Miracle: The Decades-Long Journey Behind Nanoscope’s Vision-Restoring Drug

Written By: ingridricks - Sep• 19•21
Samarendra Mohanty

On the surface, Nanoscope’s June 3rd news release announcing the remarkable vision-restoring results of its phase 1/2a clinical trial in India might sound like an out-of-nowhere miracle. But in reality, their breakthrough optogenetics drug that restored meaningful vision in 11 previously blind RP patients has been decades in the making. Without ongoing biomedical advancements combined with the rare skill set, unrelenting determination, and unwavering belief in the impossible by company president, Samarendra Mohanty, and his team, this therapy would not exist.

The Backstory

Mohanty, who grew up in a small town in India, was drawn to science because of its ability to create magic that could change the world. After graduating from the Indian Institute of Technology Delhi and the Indian Institute of Science, he began his career as a researcher and scientist at the Center for Advanced Technology in central India. It was there that he was first exposed to applications of light — especially lasers in the diagnosis and treatment of disease. His early work focused on developing devices and technology to detect oral and cervical cancers. But his focus turned to eye diseases when he read an article about optical tweezers by the inventor Dr. Arthur Ashkin, who was later awarded the Nobel prize for his discovery. 

Mohanty was soon in Germany working alongside another pioneer in the field, Professor Karl Otto Greulich, and eventually returned home to launch the first optical tweezers and laser micro manipulation lab in India.

By the time Mohanty landed at UC Irvine in 2006, he had a deep expertise in biophysics, lasers, and optics. It was a unique combo that made him the perfect fit for the newly emerging optogenetics field. Mohanty immediately began teaming with ophthalmologists and neuroscientists and set to work to crack the code that could restore vision in millions worldwide.

“Working in collaboration with neuroscientists, we developed different promoter-based opsin genes to target ganglion and bipolar cells of the retina,” notes Mohanty, who adds that this critical work was funded by the Greishaber Foundation. “I also demonstrated for the first time the non-viral delivery of opsin-genes to adult mice retinas by electroporation and spatially targeted laser delivery.” 

Like other researchers at UC Irvine, Mohanty started using monochromatic (blue) light to activate channelrhodopsin-expressing ganglion cells in the retina. But later in his career, while working as a professor at the University of Texas, he observed damage to opsin-expressing ganglion cells after chronic use of blue light. And beyond the toxicity issue, Mohanty wasn’t satisfied with just bringing back narrow bans of vision that required intense light and only resulted in restoring a patient’s ability to see shapes, shadows, and stripes. He was determined to restore meaningful vision that gave patients back their lives — which meant achieving vision restoration in a natural, broadband light environment. 

“I started fusing different monochromatic (blue, green, and red) opsins to generate broadband light sensitivity,” explains Mohanty. “However, the fused opsin gene was too large to be packed in a known-to-be-safe AAV viral vector. Therefore, we delivered such genes by a non-viral laser method, which needed further instrumentation and image guidance to be translated to humans. Moreover, I found that the broadband opsin generated by fusing three opsin-genes did not have enough sensitivity to be activated at natural/ambient light surroundings, which meant that, like narrowband opsins, we still needed an intensifier to instill vision in subjects with retinal degenerative diseases.” 

Mohanty continued to wrestle with the challenge while immersing himself in his academic work as a biophysics professor. Between faculty tasks, setting up biophysics labs, training students, teaching classes, and applying for grants, there wasn’t much time for focused research. But he continued to chip away at it — determined to give people who had been blinded by degenerative eye diseases the ability to see their world again. 

“I never considered giving up in spite of major personal and professional challenges,” says Mohanty. “I was distressed by my father’s health issues and death. I was disappointed when narrowband opsin and monochromatic light stimulation did not produce a safe and efficacious outcome. But as a self-motivated scientist and entrepreneur, I would never give up. I am passionate and driven by discovery, translation, and creating a real impact for patients with devastating neurodegenerative diseases.”

The Breakthrough

The breakthrough Mohanty and his team were searching for finally materialized in early 2016, when new MCO mutants were discovered. These opsins possessed three critical attributes: first, they were so sensitive to light that they eliminated the need for an intensifier. Second, they worked fast. And finally, they responded to broadband white or any color of visible light encountered in daily living. 

Mohanty began utilizing these MCO opsins — and that’s when the magic happened. He and his colleagues injected their newly refined optogenetics therapy into the bipolar cells of lab mice who had been blinded by RP and were able to activate them into light sensitive cells that worked in natural broadband light environments. While it was a monumental achievement, Mohanty and his colleagues immediately focused on the next step: testing the therapy in people blinded by RP. Then came serendipity. Dr. Mahapatra, a renowned ophthalmologist and retinal surgeon in India, was searching for something to help his patients with RP when he read the pre-clinical trial results published in the journal, Neurophotonics. In early 2017, he traveled to Texas to visit Nanoscope Therapeutics — which Mohanty had recently co-founded with CEO Sulagna Bhattacharya. 

“We found him to be equally passionate and truly dedicated to treat his RP patients with severe retinal degeneration,” explains Mohanty. “Since we did not have any experience in conducting a clinical study in India, Dr. Mahapatra introduced us to a CRO who could navigate and coordinate the clinical study.” 

Next Steps

Fast forward to now. Thanks to the remarkable results of the India trial, the FDA recently approved a Phase 2b clinical trial for late-stage RP that is currently underway at six locations throughout the United States. The results of that trial are expected to be delivered to the FDA in the third quarter of 2022. If the results from the U.S. trial mirror those of India, Mohanty hopes the FDA will consider an accelerated approval timeline so Nanoscope can start getting their therapy into the eyes of those of us who are clinging to the hope that we will once again be able to see our worlds.

“It means a lot to me and our team to give hope to the patients who have lost their vision due to degenerative eye diseases,” says Mohanty. “To me, it is the purpose of my life. I was very happy that some patients in our phase 1/2a study improved remarkably and that those patients/family members spoke of our therapy as extraordinary. I hope our phase 2b trial will have a similar outcome. The RP patients participating in our study will be contributing to our resolve to enable millions to see again.”

(Editor’s Note: I did everything in my power to get into this clinical trial but was excluded because of a stem cell therapy I received a few years back. I am so happy for those of you who were accepted into this trial and so hope that you will all be able to see your world again and that it will translate into a treatment that the rest of us will be able to access soon.) 

Join the conversation!

Nanoscope Therapeutics Restores Meaningful Vision with Universal Optogenetics Therapy for Late Stage RP

Written By: ingridricks - Jun• 23•21

I’ve been trying to find the words to describe the flood of emotions that have been swirling inside of me since talking with the team at Nanoscope Therapeutics about their recently announced vision restoring optogenetics therapy for late stage RP. I’ve alternated between crying, doing a happy dance, and shouting out thank you prayers to the universe. After trying to claw my way out of a dark pit for the past 17 years, I’ve finally found light. And I’m so full of hope and gratitude that I’m ready to burst.

In case you somehow missed it, Nanoscope Therapeutics, a clinical stage biotech based in Bedford Texas, issued a June 3rd press release detailing the results of their Phase 1/2a optogenetics clinical trial that took place in India over the past 2 years. By all accounts, it appears that they have cracked the code when it comes to restoring vision in late stage RP patients — regardless of gene mutation.

I’m talking functional vision restoration — not shadows, or dark blobs, or white stripes. Real, functional vision that has previously-blind patients navigating complex public transportation on their own, watching TV, reading newspaper headlines and, in one case, even riding a bike and recognizing facial features.

What’s more, their therapy isn’t dependent on implanted microchips, or on wearing external devices such as cameras or goggles. It involves a single injection of molecules into the eye targeting bipolar cells that lay just beneath the photoreceptors cells that are destroyed by RP. The therapy activates those bipolar cells, turning them into light sensitive cells that react to ambient light — the kind of natural light found in everyday living. And as far as researchers can tell, the vision restoration appears to be permanent.

“The results varied among patients, with some better than others,” notes Nanoscope’s Co-Founder and President, Samarendra Mohanty, who has been working on the development of the therapy since 2006. “But every patient who received the therapy has experienced significant improvement — both objectively and subjectively.”

The eleven patients involved in the phase 1/2a clinical trial underwent extensive testing over the course of a year, utilizing every vision-measuring metric the team could apply.

From a straight visual acuity standpoint, Mohanty said the most dramatic improvement saw a patient’s visual acuity jump from 20/2000 to 20/200. But that was just the beginning.

Patients in the trial also underwent visual field tests to measure peripheral vision, tests to measure light perception in progressively dim light conditions, and even tests to measure shape and determination accuracy. A variety of mobility tests were also performed to see how accurately a patient could identify a light source and moving objects. Dramatic improvements were seen across the board.

Along with experiencing dramatic visual improvements within four weeks of the therapy injection, Mohanty said that Nanoscope’s optogenetics therapy seeks to address another critical factor: the halting of further degeneration.

“After the photoreceptors cells die, the retina continues to degenerate,” notes Mohanty. “But we have preliminary indication of halting further degeneration and that’s very very exciting for us ”

The next step in bringing this therapy to patients everywhere is the newly announced Phase 2b clinical trial in the United States that will kick off within the next few weeks and be administered at several locations throughout the country (for more information, go to clinicaltrials.gov or contact the clinical trial coordinator, Kristen Peterson, at [email protected].). Like in India, the U.S. clinical trial is focused on late stage RP patients with bare-to-no light perception. To qualify, a patient’s visual acuity must be 20/1600 or worse.

“We wanted to start with them because we wanted to give hope to people who have absolutely no hope and have been left behind,” explains Nanoscope’s Co-Founder and CEO, Sulagna Bhattacharya, who watched her beloved uncle go blind as a child and experienced the devastating impact it had on him and her entire family. “This is why we started with RP. Our therapy also has potential to help Stargardt, and we are confident that it will also potentially benefit those with dry age-related macular degeneration. But most of the Dry-AMD patients still have a little vision left, and we wanted to start with those who were suffering the most.”

The phase 2b trial results are expected in the third quarter of 2022. If all goes according to plan, the FDA may be able to expedite the approval process so that Nanoscope can get their life-transforming therapy to patients as soon as possible.

There is too much to this story to capture in a single post. But I’ll cover it in depth in several segments over the next month. These segments will include:

  • The fifteen-year story behind the development of this breakthrough therapy and Mohanty’s determination to figure out how to restore vision in ambient light — which was key in activating the bipolar cells and restoring meaningful vision
  • The remarkable journey of Bhattacharya, who has devoted her life to finding a cure for blindness after her uncle lost his eyesight — even while enduring unimaginable loss and grief
  • The team’s commitment to making this life-changing therapy affordable and accessible to patients everywhere, and the uphill challenge to achieve this

Like all of you who have been following this blog since its inception in early 2013, I’ve refused to believe that I am destined to live in a world of darkness. Even after my eyesight took a nose-dive in 2018 and my retinal specialist told me it was time to transition to blindness, I’ve maintained my determination to see. Now, though there is still a ways to go, it feels close enough to touch. I am so grateful to all of the scientists and researchers out there who are devoting their lives and careers to bringing back our eyesight and our lives. And I’m making it my mission to do everything I can to raise awareness and help get these life-changing treatments out to the world.

Join the conversation!

Chemically Induced Retinal Cells Offer Vision Restoration Hope for RP

Written By: ingridricks - Apr• 15•21

Dr. Sai Chavala

I’ve been in hiatus for a couple of years because—between breast cancer and a sudden, dramatic drop in vision that now hovers around light perception—I felt like I had been smashed in the face with a two-by-four. But like all of you who are determined to see your family’s faces and the world around you, I’ve continued to believe that an answer will materialize. And the new chemically induced retinal cell therapy developed by ophthalmologist and researcher Dr. Sai Chavala and his team might just be the miraculous, vision-restoring breakthrough we’ve all been channeling.

Before I get to the remarkable story behind this potentially game-changing therapy, here’s what I know you all want to know: Through a combination of cutting-edge research, trial and error and unrelenting determination, Dr. Chavala and his team have managed to convert ordinary human skin cells into functioning retinal cells by applying a proprietary chemical cocktail that serves as a reprogramming mechanism. And, at least in mouse models, they have been able to restore some sort of vision in completely blind mice.

Though it’s still in the pre-clinical trial phase, what this scientific breakthrough means for those of us suffering from RP is potentially so holy-crap-amazing it has taken the scientific world by storm–with the research data first published in the premier scientific journal, Nature, last year.

Here is what makes it so astounding:

  1.  Easy, affordable access to cells. Unlike stem cells, which can be hard to access and controversial, this cell therapy relies on a person’s own skin cells that can be harvested through a quick five- to ten-minute biopsy.
  2.  Because the cells aren’t first being converted to stem cells—which in theory then mimic a retinal cell or any other kind of cell—there is no concern about the stem cell taking on the wrong, potentially harmful characteristics. There is also no need for a significant portion of photoreceptor cells to still be alive in order for the stem cells to take hold. This is because the cells being injected into the patient’s eye have already been converted to retinal cells.
  3. This potential vision-restoring therapy isn’t specific to a gene mutation and isn’t limited to a specific disease stage. In other words it’s application is for all of us.

The Backstory

Dr. Chavala started out as an ophthalmologist who planned to take over his dad’s eye practice in rural Missouri when he retired. But then he did a stint at the renowned Cleveland Clinic, where he was introduced to the research side of the equation, and was immediately intrigued. He realized he was in a unique position to merge his clinical expertise with breakthrough research that he hoped would result in vision-restoring therapies for patients suffering from blinding eye diseases.

“It was out of sheer frustration and helplessness that I pursued additional training in basic science,” he said. “The decision came from perpetually explaining to patients, some that had traveled from other countries to the world-renowned Cleveland clinic for a shred of hope, that there was simply nothing that could be done to improve their vision. The tears and dismay that ensued were heart breaking.

“As a trained physician, it was not appealing to take this unconventional departure from clinical training,” he added. “But I felt it was necessary to be able to have the skill set to create next generation medical therapies for eye disease.”

With the blessing of his boss at the Cleveland Clinic, Dr. Chavala went for it.

That was in 2009, when all the top scientific minds were focused on embryonic stem cells. Dr. Chavala read a cover story about it in a Time magazine article and began contacting all the scientists featured in the story.

“I got no response,” he said. “I had no research training and they were at the top of their game. I was going to give up, but then I went to a lecture for a world-renowned oncologist who was conducting cutting-edge stem cell research.”

Dr. Chavala Googled the oncologist and found his phone number on the internet. When he called the number, the doctor picked up.

“I gave him my heartfelt speech on why he had to take me into his lab and he agreed. It changed my entire path.”

While it might sound weird that Dr. Chavala would work with an oncologist, that’s where all the research dollars were earmarked, and it turns out that the parallels between stem cell therapies to treat cancer and eye diseases were striking. Dr. Chavala began cherry-picking applications from the cancer research to apply to the retina. After receiving extensive research training in New York, he underwent surgical training at Duke and eventually landed at the University of North Texas, where he received an NIH grant to start his own research experiments. In the meantime, breakthroughs in cell therapies had advanced to the point that skin cells were now being used as a replacement for embryonic stem cells which was the game changer Dr. Chavala’s team was looking for.

He and his team at the University of North Texas Health Science Center scoured published research as a starting point and then began experimenting with what felt like countless variations of chemicals and growth factors.

“We failed many times, to the point that we were going to give up,” admitted Dr. Chavala. Then it happened. The cells they were reprogramming turned green, which meant they had converted into retinal cells. “I was in disbelief, but I was cautious,” he said.

The next step was to inject the new retinal cells into mice that had lost all photoreceptor cells due to RP and were completely blind to see if they could actually work as functioning retinal cells. At the two-week mark, Dr. Chavala said there was no improvement. But three weeks after the chemically induced retinal cells were injected, his team noticed that the pupil was responding. Buoyed on by this accomplishment, they ran other tests with the mice that demonstrated that, at the very least, the mice could now differentiate between light and dark. This continued through the twelve-week mark—illustrating that synaptic connections were being made to the retina and that these cells were continuing to survive.

“After three months, we wanted to prove to people that the cells were doing something,” noted Dr. Chavala. “We euthanized them and sectioned the eyes. Sure enough, the cells were still green. Even after the chemicals were gone, they were still retinal cells.”

Next Steps

CiRC Biosciences, which was started by Dr. Chavala in an effort to get the retinal cell therapy to market, was recently acquired by Paragon Biosciences, which focuses on advancing life-changing therapies.

Eric Bauer, Executive Director, Clinical Operations Tim Cunniff, PharmD, Executive Vice President, Research & Development  Steve Wanaski, PhD, Senior Vice President, Research & Exploratory Development  Kevin Scoby, Assistant Vice President, Portfolio Management

Eric Bauer | Executive Director, Clinical Operations
Tim Cunniff | PharmD, Executive Vice President, Research & Development
Steve Wanaski, PhD | Senior Vice President, Research & Exploratory Development
Kevin Scoby | Assistant Vice President, Portfolio Management

Tim Cunniff, Executive Vice President of Research and Development for Paragon, said the first step was achieving orphan drug designation from the FDA. This acknowledgement of the potential benefits of the retinal cell therapy for RP provides seven years of exclusivity (two years longer than other drug designations) so CiRC Biosciences has the necessary time to conduct the investigational research and clinical trials required to bring it to market. The next step, said Cunniff, is to conduct all the pre-clinical trial work required to establish safety and efficacy.

“We won’t just be replicating Dr. Chavala’s work,” noted Cunniff. “We will do experiments to determine if the order of chemicals added, the quantity of chemicals, or how long the chemicals are held in process improve results. It’s about optimizing everything.”

The investigational research is expected to take two years, with phase 1 and 2 clinical trials slated to begin in early 2023. That’s when we will begin to learn if this is, in fact, the key to reversing blindness and restoring sight in humans—regardless of how far our RP has advanced or what gene mutation we have.

There are still a lot of unknowns, such as how much vision can be restored and how long each dose of the chemically induced retinal cells will last. While there is still a ways to go before we’ll have the answers all of us are desperate to receive, the team at CiRC Biosciences, which will be conducting trials focused on both vision restoration and blindness prevention, are doing their best to fast track the process.

“We are very excited and hope to have this therapy on the market in seven years, which is very quick for these types of therapies” said Cunniff, noting that every person on his small team at Paragon—all of whom have deep expertise in the pharmaceutical and regulatory space—have put in personal funds to support CiRC Biosciences and will be intimately involved. “We know that reversing and preventing blindness is the holy grail and we are working as fast as we can. We are putting in the work on the front-end with the formulations and doing the robust studies necessary to save time in the long run.”

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