Place an Ad | Subscribe | Advertise With Us

Church welcomes mayor for Black History program

Photo

Special to the News

This weekend, Salem’s Pleasant View Missionary Baptist Church will host Tuskegee Mayor Johnny Ford as the guest speaker for its 2008 Black History Month Celebration.

Text size: small | medium | large

By Donathan Prater

Published: February 22, 2008

It’s fair to say Tuskegee Mayor Johnny Ford knows a thing or two about history.

After all, for most of his life, he’s been a pioneer of sorts in contributing to it as a native of the city he describes as a “citadel of black culture.”

This weekend, Salem’s Pleasant View Missionary Baptist Church will host Ford as the guest speaker for its 2008 Black History Month Celebration.

Ford was elected in 1972 as Tuskegee’s first black mayor and served in the position for 24 years. He returned to the mayor’s office in 2004.

The opportunity to speak at PVMBC is one that Ford looks forward to.

“From the legacy of the Tuskegee Airmen, to the accomplishments of Booker T. Washington. to the scientific contributions of George Washington Carver, we are reminded of our rich history as African-Americans - not only during Black History Month but year round,” Ford said.

In discussing the contributions of blacks to American history, Ford is also expected to commend Sarah W. Thomas, PVMBC program chairperson, for her efforts in raising funds and awareness for research and a cure for sickle cell anemia.

Thomas, the founder of East Alabama Sickle Cell Foundation, took up the cause of finding a cure for the illness after it claimed the life of her son, Todd, in the mid-1970s.

Thomas credits former Gov. George Wallace with being instrumental in helping allocate some of the first funds for sickle cell research in the state and declaring the month of February as State Sickle Cell Month in memory of her son.

While the mayor will be speaking to the congregation on past contributions of blacks, Ford, who has also served on the board of the East Alabama Sickle Cell Foundation, encourages the community to help carry on that legacy through the next generation.

“We must continue to teach our children about the value of education, avoiding drugs and violence and making solid life choices,” Ford said.

“I want to challenge our community to remain focused,” said Ford, who mentioned the exciting time we live in politically in which both a black and a woman are presidential candidates.

“Many of the political freedoms we enjoy now can be directly attributed to the struggles of the Civil Rights Era,” Ford added.

Reader Reactions

Posted by ( Asclepius ) on February 23, 2008 at 9:21 am

This drug is a major advancement in the treatment of sickle
cell disease unfortunately it is not available in the U.S..
Although the compound has been granted orphan drug status
by the FDA and the regulatory body of the European Union,
to date investigational drug applications for the approval
process have yet to be submitted. Getting a drug approved
in either area is extremely expensive. Until there is
funding available to proceed with the FDA and EU
applications it will be difficult for non-Nigerians to
obtain the drug.

I do say difficult but it is not impossible. If you have a
hematologist or hemoncologist who is willing to put fourth
the effort there are special dispensations available
through the FDA for the importation of unapproved drugs on
a compassionate use basis.

“Expanded access program (EAP). EAPs are typically designed
to provide widespread access to a drug that has proven
efficacy in clinical trials but is still awaiting FDA
approval. They’re similar to standard clinical trials
with
a specific treatment plan and certain FDA requirements, but
they have looser patient eligibility criteria. More than
23,000 U.S. cancer patients enrolled in an EAP for Iressa
before it was FDA-approved, for example.”

“Single patient use. This program offers an experimental
drug to an individual patient, rather than a group. The FDA
approves these uses on a case-by-case basis. Decisions are
based on other treatments already available and information
about the drug’s efficacy and potential toxicities.”

http://www.curetoday.com/backissues/v3n3/departments/specialreport/index.html

To date I have no knowledge that anyone has sought any
single use or expanded access from the FDA for Nicosan.
Unfortunately regardless of the dissemination of this
information thus far no one has put forth the effort to
obtain the drug for use.

If just one person would start the ball rolling with a
caring and concerned medical practitioner it could open up
the drug for wide spread use by tens of thousands of
patients across the U.S. Unfortunately thus far the general
response I receive is that people don’t believe that their
physician would be interested in going to this sort of
effort nor do they themselves seem to be inclined to seek
the use of a treatment that could potentially end their
crises.

There has to be at least one physician out there who has
enough care and concern for his patients to be willing to
put forth the effort necessary to obtain this medication
legally. I urge anyone who is effected by sickle cell to
approach their physicians with this information and attempt
to obtain this treatment not only for themselves but for
all patients who could potentially benefit from it’s use.

We already know the benefits of the treatments available in
the U.S. and the E.U.. In many cases they are only
marginally effective or in the case of hydroxyurea cause
side effects so serious that many choose not to use it as
treatment. Here we have an opportunity to use a treatment
that has been shown to be highly effective, eradicating
crises in the majority of patients and reducing crises by
50% in the most refractory cases.

Although the clinical trial group was what the casual
reader might interpret as quite small it is common for
drugs which fall into the orphan drug category to use small
sample groups. Many orphan drugs have been approved based
on very small phase II and phase IIb clinical trials in the
U.S. In the case of FDA fast track status, a drug may be
approved during phase II trials if the drug shows
significant advantage over current approved therapies for
life threatening illness.

Fast Track Designation is a program that, if granted, is
designed to facilitate the development and expedite the
review of new drugs, thereby allowing the FDA to approve
drugs used to treat a serious condition or a
life-threatening disease with less safety data following
the conclusion of phase II studies, rather than phase III,
the normal practice.

The main criterion for a Fast Track Designated drug is the
potential to treat a life-threatening illness or fill a
major unmet medical need. Fast Track may be submitted with
the IND or at any time during the clinical development of
the drug. The Fast Track designation may allow a company’s
application to follow Priority Review, Standard Review, or
a Rolling Review of the application.

http://www.fda.gov/CbER/gdlns/fsttrk.pdf

Nicosan by Western standards is an extremely inexpensive
drug. It is available in Nigeria without prescription at
$23/month for adults and child doses at $18/month.

Company and product website.

http://xechemnigeria.com/products.htm

I sincerely hope that you find this information helpful. I
would encourage you to forward and post this information
to any person, blog or website where persons effected by
sickle cell anemia can have access to this information.

Feel free to write me with any questions or you may have.

Report Inappropriate Comment

Posted by ( Asclepius ) on February 23, 2008 at 9:19 am

NICOSAN for the Treatment of Sickle Cell Disease

There is a relatively new treatment for sickle cell being
produced in Nigeria by an American company called
NICOSAN®,
it’s proprietary name is NIPRISAN® . It was developed on
the premise of traditional Nigerian plant based medicinal
practices for the treatment of sickle cell disease.

It has been tested through phase IIb clinical trials and
found to be highly efficacious. Phase III trials have yet
to be completed however it was approved for sale in Nigeria
based on phase IIb trials and toxicity studies which showed
it to be safe and non-toxic.

Double-blind, placebo-controlled, randomised cross-over
clinical trial of NIPRISAN® in patients with Sickle Cell
Disorder

http://www.sciencedirect.com/science?_ob=ArticleURL&_udi=B7GVW-4DS346T-1S&_user=10&_rdoc=1&_fmt=&_orig=search&_sort=d&view=c&_acct=C000050221&_version=1&_urlVersion=0&_userid=10&md5=211981d545303693affebb8c012d2cac

Efficacy of Niprisan in the prophylactic management of
patients with sickle cell disease

http://www.sciencedirect.com/science?_ob=ArticleURL&_udi=B6VS8-43DFJCH-G&_user=10&_rdoc=1&_fmt=&_orig=search&_sort=d&view=c&_acct=C000050221&_version=1&_urlVersion=0&_userid=10&md5=10528ecbab3ec7e977301fb9f2688ef6

NIPRISAN—Nix-0699 Toxicity Studies

http://findarticles.com/p/articles/mi_m0EIN/is_2004_April_27/ai_n5999832
http://www.biospace.com/news_story.aspx?StoryID=15890720&full=1

Niprisan (Nix-0699) improves the survival rates of
transgenic sickle cell mice under acute severe hypoxic
conditions

http://www.blackwell-synergy.com/doi/abs/10.1046/j.1365-2141.2003.04536.x?journalCode=bjh

NIPRISAN Case, Nigeria
A Report for GenBenefit (2007)

http://www.theparliament.com/NR/rdonlyres/F46A1A12-0A1A-41DA-9F5D-A11486CA9BFA/0/Nigerian_Case.pdf

Report Inappropriate Comment