November 20, 2014 by

Roberta F. Shapiro DO, FAAPM&R: “A New York Doctor’s Path to Panama” – A Stem Cell Therapy Video Lecture

Special Guest Speaker, Roberta F. Shapiro DO, FAAPM&R speaks about: “A New York Doctor’s Path to Panama” at the Stem Cell Institute’s Stem Cell Therapy Public Seminar in New York City on May 17, 2014.

Dr. Shapiro discusses how she discovered the Stem Cell Institute and why she started referring her patients to Panama for stem cell therapy.

Dr. Shapiro operates a private practice for physical medicine and rehabilitation in New York City. Her primary professional activities include outpatient practice focused on comprehensive treatment of acute and chronic musculoskeletal and myofascial pain syndromes using manipulation techniques, trigger point injections, tendon injections, bursae injections, nerve and motor point blocks. Secondary work at her practice focuses on the management of pediatric onset disability.

She is the founder and president of the Dayniah Fund, a non-profit charitable foundation formed to support persons with progressive debilitating diseases who are faced with catastrophic events such as surgery or illness. The Dayniah Fund educates the public about the challenges of people with disabilities and supports research on reducing the pain and suffering caused by disabling diseases and conditions.

Dr. Shapiro serves as assistant clinical professor in the Department of Rehabilitation and Regenerative Medicine at Columbia University Medical Center.

Filed Under: News, Roberta Shapiro DO, Stem Cell Therapy, Video - Stem Cell Therapy Tagged With: , , , ,
November 20, 2014 by

The Lip TV News: Neil Riordan, PhD on Exploring New Stem Cell Treatments for MS, Arthritis, Autism and More

Stem cell treatment and research towards curing illness–from multiple sclerosis to spinal injury–is detailed by Dr. Neil Riordan. The American medical industry, obstructions to research in the states, misconceptions about stem cells, and the details about the treatment process are explained–and we look at video of patient recovery and speculate at what the future could spell for stem cell treatment and research in this Lip News interview, hosted by Elliot Hill.

GUEST BIO:
Dr. Neil Riordan is the founder and Chairman of Medistem Panama, a leading stem cell laboratory and research facility – located in Panama City. His institute is at the forefront of research of the effects of adult stem cells on the course of several chronic diseases. Dr. Riordan has more than 60 scientific articles in international peer-reviewed journals. In the stem cell arena, he and his colleagues have published more than 20 articles on Multiple Sclerosis, Spinal Cord Injury, Heart Failure, Rheumatoid Arthritis.

Filed Under: multiple sclerosis, Neil Riordan Phd, Neil Riordan PhD, News, Rheumatoid Arthritis, Spinal Cord Injury, Stem Cell Lecture Videos, Stem Cell Research, Stem Cell Therapy Tagged With: , , , , , , , , , , , ,
May 6, 2014 by

Colorado MS patient returning to Panama for more stem cell therapy

By Travis Khachatoorian
Created: Mon, 05 May 2014 10:21:00 MST
Updated: Mon, 05 May 2014 11:27:10 MST

CLIFTON, Colo. – Even with all the advances in medical sciences over the years, multiple sclerosis remains mysterious in both causes and symptoms. There is no known cure for the disease, but one Clifton resident isn’t waiting on the US government anymore and is planning to fly to Panama for a stem cell therapy.

Pam Claypoole was diagnosed with MS almost a decade ago and has slowly lost the feeling in her legs and right arm. She said since the FDA currently doesn’t approve any stem cell therapies for her disease, she’s planning a second trip to Panama in hopes to improve her condition.

Claypoole said she’s made one trip to the Stem Cell Institute in Panama more than a year ago and was amazed by the effects.

“I felt it made a big difference for me right away,” said Claypoole. “My walking was better, the feeling in my feet was better, I had more energy.”

She emphasized her treatment doesn’t involve unborn fetus stem cells but rather the stem cells taken from healthy birthed babies umbilical cords.

Her family is currently planning a live auction on May 14th at the Western Slope Cattleman’s Livestock Auction in Loma. The event starts at 6 pm, and they’re hoping to collect $20,000 dollars to fund Pam’s therapy in Central America.

more…

Filed Under: Multiple Sclerosis, Multiple Sclerosis, multiple sclerosis, Multiple Sclerosis, News, Patient Stories, Stem Cell Institute Panama, Stem Cell Therapy, Video - Stem Cell Therapy Tagged With: , , , , , , , , ,
April 10, 2014 by

“I am riding my bike 10 miles a day, swimming, walking…all virtually PAIN FREE!” – Debra Deuble

We received this message from Debra Deuble yesterday. Debra gave us the ok to share it with everyone.

“I am a stem cell recipient from your clinic in Panama! I am grateful every day that I had this done. It has been over a year and I have not been on any medications and I feel great! I am riding my bike 10 miles a day, swimming, walking…all virtually PAIN FREE! I feel like I have had the fountain of youth! I was diagnosed with severe Rheumatoid Arthritis. I was 37 when I had symptoms and 46 when diagnosed. Was on meds for 7 years and nothing helped. So glad I found your website in my search for a cure!!”

Filed Under: Autoimmune Diseases, Patient Stories, Rheumatoid Arthritis Tagged With: , , , , , ,
March 12, 2014 by

Neil Riordan PhD on stem cell expansion in stem cell therapy

Stem Cell Pioneers featured Dr. Riordan in its February installment of “Ask the Doctor”, a monthly segment that features stem cell scientists and doctors answering questions from readers about stem cell therapy.

Over the next several days, we will share these questions and Dr. Riordan’s answers with our readers.

Question: Are there some conditions such as neurological ones that respond better when the cells are greatly expanded? Is a high quantity essential for success or is that something that may be more of a selling point at some clinics? I have also seen this advertised for COPD and other conditions. It’s almost like the more cells the better, but I would like your opinion.

Dr. Riordan’s Answer: That really depends on the quality of the cells after expansion. If they are still robust, not senescent, and still have a good secretion profile, then the more the better may be useful up to a point. If you take a small pool of starter cells and expand them to exhaustion, then I don’t think you are going to have a very good product. The MSCs used in Panama are not expanded beyond passage 5—a point at which there is no senescence in the population and they have a robust cytokine secretion profile. In order to use only cells that meet our release criteria, cells from approximately one (1.2 to be exact) out of 10 donated umbilical cords are used.

Contrast that to cells from a patient’s own fat tissue that are expanded. Firstly, the starting cells may, and many times are not very robust—they secrete little or no beneficial cytokines or chemokines, and must be expanded to hilt in order to hit the cell number. Please see my answer to number 7 for more on this subject.

This brings up a slightly different, yet related topic. There has been a lot of talk at recent meetings about more defined endpoints for the cells being used, and I couldn’t agree more. There are MSCs from bone marrow, menstrual blood, fat tissue, umbilical cord (even different parts of the umbilical cord—around the blood vessels, from the Wharton’s jelly, from the subepithelium, from the cord blood itself—which are most likely contaminants from a bruised placenta rather than the blood), teeth, amniotic membrane, amniotic fluid just to name sources in the “we didn’t mess with mother nature” adult stem cell world. Add to that the infinite variables when you consider the age and physical condition of the donor, particularly when using adipose or bone marrow as a source material and we, as a field, could be saying almost anything by using the term, “mesenchymal stem cell.” I think it is time that there is standardization in the field beyond the current definition of expressing/not expressing certain surface markers and the ability to differentiate into fat, bone, and cartilage. That standardization could come from using endpoints such as “remaining proliferative capacity (the number of doublings achievable in culture from the treatment cell bank), the secretome, even if there is standardization of one or two molecules, such as HGF, or one of the prostaglandins.

In the future I believe the field will take it a step further by measuring, even by a surrogate marker, the potential effects of the cells on the target condition. In the case of autoimmunity the cells and their secretions could be tested for their capacity to modulate the immune system. In the case of inflammatory conditions, the cells and their secretions could be tested for the ability to control or block inflammation.

Filed Under: Adipose Stem Cells, Adult Stem Cells, Amniotic Membrane, Mesenchymal Stem Cells, neil riordan, Neil Riordan Phd, News, Stem Cell Institute Panama, Stem Cell Research, Stem Cell Therapy, Stem Cells, Uncategorized Tagged With: , , , , , , , , , , , , ,
March 11, 2014 by

Neil Riordan PhD on Peri-lymphatic Stem Cell Treatment for Multiple Sclerosis

Stem Cell Pioneers featured Dr. Riordan in its February installment of “Ask the Doctor”, a monthly segment that features stem cell scientists and doctors answering questions from readers about stem cell therapy.

Over the next several days, we will share these questions and Dr. Riordan’s answers with our readers.

Question: I have heard from patients that you are doing intralymphatic stem cell injections. I think there are a lot of IntraLymph studies on other things like allergies, but none on stem cells that I can find. What is the reasoning behind this new route of administration? If stem cells get stuck in the lungs and we worry about that, why inject them directly into the lymph system where they would go to the spleen?

Dr. Riordan’s Answer: The goal of our treatments umbilical cord mesenchymal stem cells for patients with multiple sclerosis really has nothing to do with repairing the damaged or destroyed myelin in the lesions found in the brain and spinal cord. Because multiple sclerosis is first and foremost an autoimmune disease our goal is to address the immune dysfunction. At the root of the disease is a pool of immune cells called T-cells, which actively proliferate, cross the blood brain barrier, and attack myelin. Our primary goal then is to interfere with myelin-specific T-cell reproduction (something called “clonal expansion’). Mesenchymal stem cells (MSCs) have been shown in multiple studies to have the capacity to block this so-called clonal expansion of activated T cells. In a way MSCs immunosuppress, but unlike some drugs that suppress the immune system this specific blocking of activated T cells does not quash the entire immune system—the cells and their secretions only block the clonal expansion. Other drugs that suppress the immune system—for example hydrocortisone—have an effect on the entire immune system, which can increase the risk of the recipient to infectious diseases and even some cancers.

If it were the goal of the treatment to induce remyelination then certainly the route of delivery would be of greatest importance. You would want for the cells (or whatever proposed remyelination agent) to be as close to the lesions requiring the repair as possible. So I understand the rationale for the question.

In my opinion it will be difficult to successfully treat multiple sclerosis by remyelination alone because if you do not address the immune problem you will continue to lose myelin. Therefore, getting the cells to the lesions for myelin repair is not particularly important. Further support for this opinion is that there is very good evidence that the body has the innate ability to regenerate myelin without intervention. There are two good examples of this. The first example comes from a condition called Guillain–Barré syndrome. The syndrome is an autoimmune disease that results from an immune attack on the myelin of peripheral nerves. There is an ascending paralysis and the condition can be life threatening if the paralysis gets high enough to affect breathing. It is treatable and generally temporary. In 80% of the patients the underlying nerves are not irreparably damaged and there will be no long-term neurologic symptoms. 20% experience permanent nerve damage because the axons of the nerves are damaged. The good news is that the disease is temporary. The better news is that in the mild cases in which the axons were not destroyed, complete remyelination occurs—the body has the capacity to restore myelin.

The second example comes from a phenomenon seen with serial MRI images of the brains in people with MS. Fifty percent of these low intensity lesions known as “black holes” revert within one month of appearance, indicating that remyelination has occurred spontaneously.

Further support for the “treat the immune system and not the Central Nervous System” in MS comes from the work of several groups, including Northwestern University who are using chemotherapeutic “conditioning”, ie. wiping out the immune system (and the by-standing hematopoietic stem cells) followed by bone marrow reconstitution using previously harvested bone marrow stem cells. There are published results of many cases improving without anything having been done to address the myelin loss.
To the question of intra-lymphatic injections: There has been no work on “intra-lymphatic” injections. We are looking into peri-lymphatic (near the lymph nodes) injections of huMSCs for patients who are refractory to intravenous treatment.
Here is a little background on this subject: Dr. Arnold Caplan of Case Western Reserve, the scientist to first describe mesenchymal stem cells, was in Panama last year consulting with us. He also presented at a conference that we cosponsored. In one of my discussions with Dr. Caplan he casually mentioned that whenever they injected mesenchymal stem cells into the abdominal cavity of animals that did not have an active inflammatory process in there in the cavity the MSC’s would automatically go to the abdominal lymph chains. They were able to determine this because they use cells that were labeled with the florescent probe. I found this very interesting given that the 70-80% of the immune cells of your body reside in the abdominal cavity in and around the intestines.

The rationale for peri-lymphatic treatment is relatively simple. Firstly, the goal of therapy in autoimmune disease is to induce immune tolerance in the face of immune intolerance. The majority of the immune cells are found in the lymphatic (which includes the lamina propria) system of the gut. MCSs will, when lacking a more compelling inflammatory signal, migrate to the lymph nodes. Once in the lymph nodes they will migrate and interact with the immune cells (T-cells and T-cell priming dendritic cells). We know for a fact that MSCs interfere with dendritic cell priming of T-cells.

My book will be coming out in April. It will go into greater detail on this subject and many more. There are case histories as well as treatment protocols and rationale for each condition. Information about how to get the book “Mesenchymal Stem Cells: Nature’s Pharmacy” will be on www.Riordanbooks.com, as well as on www.amazon.com.

Filed Under: multiple sclerosis, Neil Riordan Phd, News, Stem Cell Institute Panama, Stem Cell Therapy Tagged With: , , , , , , , , , ,
January 8, 2014 by

Stem cell therapy for COPD

Email from a COPD patient on Jan 8 to Dr. Paz. We have removed this patient’s name since she has not yet informed her doctors in the US about her treatments in Panama. She received multiple intravenous injections of human umbilical cord-derived mesenchymal stem cells over the course of several days.

From: REDACTED
Subject: Re: Surveys
Date: January 8, 2014 at 7:48:49 AM EST
To: Jorge Paz Rodriguez

Dr. Paz,

I definitely feel there is an improvement from the 1st to the 2nd treatment. I feel much stronger and feel that I am able to function with a better quality of life. Prior to my 1st and 2nd treatments it was hard for me to keep up with the housekeeping, cooking, laundry and going out to the store for groceries was very hard for me to do. I have more energy to complete the task at hand now. I am able to walk longer distances without having to sit and rest and not getting as winded walking. Going up and down stairs is easier for me to do. I do feel I am making improvements with each treatment.

I have health insurance again and the Dr. here was wanting to do a physical with a chest X-ray to see the change in my COPD since my last X-ray a couple of years ago. I thought I could send you the X-ray on CD so you could compare the X-ray to what I originally sent you. I have not shared with the Dr.’s or anyone here about my treatments in Panama.

Please let me know about the Survey and if you think I should do the X-Ray and send it to you.

Thank you,

REDACTED

Sent from my iPad

Filed Under: COPD, COPD, News, Patient Stories Tagged With: , , , , , , ,
December 10, 2013 by

Stem cell therapy for traumatic brain injury – Oswaldo Tapanes

Oswaldo Tapanes received multiple injections of human umbilical cord-derived mesenchymal stem cells and his own bone marrow-derived stem cells over the course of a month both intrathecally (into the spinal fluid) and intravenously at the Stem Cell Institute in Panama. Here is what Mr. Tapanes had to day about his progress thus far:

My name is Oswaldo Tapanes. I have a traumatic brain injury; diagnosed in June 2005.

What symptoms did you have before stem cell therapy?

I couldn’t move my left arm. My vision was pretty bad. My speech is worse than it is now. I could only make sounds. My balance was very, very bad and that’s about it.

What improvements have you noticed since your stem cell treatments?

My speech is better. My eyesight is better. My arm coordination is better. My balance overall and better overall well-being.

How has this treatment changed your life?

It improved my quality of life, so much so that I’ve returned now for a second treatment.

What would you tell others who are considering this treatment?

I would say obviously, do your own research but from my point of view, it’s very safe. The medical science is explained. Everything is there on the web site if you look at it and do your homework. I wouldn’t hesitate coming. If I knew before, I would have came earlier.

Filed Under: News, Patient Stories, Patient Testimonials, Stem Cell Therapy, Traumatic Brain Injury, Traumatic Brain Injury, Video - Stem Cell Therapy Tagged With: , , , , , , , , ,
December 5, 2013 by

Heart failure patient has 3 normal EKGs after stem cell therapy

I was diagnosed 20 years ago. My heart was stopped up. I have 11 stents in my heart. When they put in (stents) nine, ten and eleven they blocked an artery and caused me to have a heart attack. Then 4 years later, I went to the doctor and he did an EKG and he said he needed to do a nuclear scan. That was in May 2011. In July of 2011 he did a nuclear scan and then called me and told me there was nothing else he could do for me.

A friend of mine in Corpus Christi told me about stem cells in Panama. So I checked into it and I came down in October of 2011 and had a treatment.

[Mr. Gray received multiple doses of human umbilical cord-derived mesenchymal stem cells over the course of several days.]

I didn’t feel anything for 30 days. Then I started feeling better and really felt good. I went to the doctor in January of 2012. He did an EKG and walked in and said, “What have you done?” I said, “What are you talking about?” He said, “You have a normal EKG. You’ve never had one of these before.“ So I asked my wife, “Do you think I ought to tell him?” This was in St. Dominic’s Hospital in Jackson Mississippi; the one that had caused me to have the heart attack. So I asked her, “Reckon I ought to tell him I had got stem cells?” She said, “Yes.” So I told him. He looked like I had cut his throat. He was white as a sheet and he wanted to know, “How did they do it?” and I told him.

Since then I have had 3 normal EKGs. The last one was about 2 months ago.
Well, I had another treatment about 11 months later and it fixed my kidneys the second time. The first time it fixed my heart. It didn’t do anything else but then the second time it fixed my kidneys. I had horse shoe kidneys and I was operated on when I was 33 years old, 35 years old and now I’m 69. My kidney had grown together and my kidneys have been bad my whole life but now they’re fine.

Filed Under: Heart Disease, Heart Disease, Heart Failure, Heart Failure, Heart Failure, News, Patient Stories, Patient Testimonials, Stem Cell Therapy, Video - Stem Cell Therapy Tagged With: , , , , , , , ,
November 14, 2013 by

Stem Cell Therapy for Relapsing-Remitting MS

Bonnie, who suffers from relapsing-remitting multiple sclerosis (MS) received a combination of human umbilical cord mesenchymal stem cells and adipose-derived cells administered daily over the course of 5 days.

Just wanted to send an update as I am really excited! I received my very first stem cells on 10/22/13, it has been less then a month and I am happy to report that I have tons more energy by balance is improving every day, I have no more foot drop and not even a healing I was looking for but I put my glasses on the other day only to find they made my vision blurry I didn’t need them, I am already saving for my next treatment! I can’t thank you all enough as I feel like I have a future with my 5 small children now, if you ever need someone to talk to future patients I would be happy to scream my praises! Looking forward to more and more improvement!

Sincerely,
Bonnie Barrington

For more information about MS clinical investigations at the Stem Cell Insitute: Stem Cell Therapy for Multiple Sclerosis

Filed Under: Multiple Sclerosis, Multiple Sclerosis, Patient Stories, Stem Cell Therapy Tagged With: , , , , , , , , ,
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