New drug may be best treatment for leukemia yet

This is the headline from CNN's site June 20, 2013. The following is the actual story text from CNN (just in case the link becomes unavailable).

It's called ibrutinib, and it's a potential breakthrough in treating chronic lymphocytic leukemia (CLL) that could leave patients with fewer side effects than chemotherapy.

It's called ibrutinib, and it's a potential breakthrough in treating chronic lymphocytic leukemia (CLL) that could leave patients with fewer side effects than chemotherapy.

In research published in the New England Journal of Medicine (NEJM), scientists report that the experimental drug, which differs from broadly acting chemotherapy agents by specifically targeting certain cancer-causing processes, significantly prolongs the life of patients.

Ibrutinib is currently being tested on tumors that target the body's immune system, such as CLL and mantle cell lymphoma (MCL).

CLL is the second most common form of leukemia among adults in the U.S., and about 15,000 Americans, most of whom are elderly, are diagnosed with the blood and bone marrow cancer every year.

The drug is the first to bind to and block the activity of a protein known as Bruton's tyrosine kinase (BTK), which plays an important role in helping immune cell tumors, which develop from abnormally growing blood stem cells, to grow.

Once ibrutinib binds to the immune system's B-cells, it prevents tumors growing in these cells from signaling for the nutrients they need to grow and divide. According to the study, the drug doesn't seem to affect the body's T-cells, as chemotherapy agents do, so patients experience fewer side effects.

TIME: On the horizon at last, cancer drugs that harness the body's own immune system

Early work on animals showed that the experimental drug effectively shut down tumor cell division, so the researchers tested the compound on 85 CLL patients who had all tried and failed to respond to at least two other anti-cancer treatments. Some even harbored genetic mutations associated with particularly aggressive forms of CLL that typically lead to death within two years of diagnosis.

The patients were randomized to take one of two different doses of an ibrutinib pill a day. After nearly two years of treatment, 71% of this hard-to-treat group had responded with slower tumor growth, and at 26 months, 75% showed no additional progression of their cancer. At the end of the study period, 83% of the participants were still alive, and most of the patients only complained of diarrhea and fatigue.

"This is truly a breakthrough drug for CLL. I have been a CLL specialist since 1997, and we have not had a drug like this come into the field yet," says study author Dr. John C. Byrd, the director of the division of hematology at The Ohio State University Comprehensive Cancer Center.

"The most common thing I have heard patients say is that it brings their disease under control and makes them feel how they did before their cancer. I've heard that at least a dozen times."

The scientists and patients were most encouraged by the fact that the the drug helped them to enjoy a longer period of time, on average, in which their tumors remained stable and didn't progress, than they they had while using chemotherapy agents.

The MCL patients showed similarly positive results. MCL is an aggressive form of non-Hodgkin lymphoma that generally doesn't respond to existing chemotherpay, immune-based treatment or stem cell transplants.

But in a separate study also appearing in NEJM involving 111 advanced MCL patients, about 68% of the participants responded to ibrutinib and 58% were alive after 18 months on the therapy. The response rate was encouraging since the last agent to treat MCL was approved by the Food and Drug Administration (FDA) with a 30% response rate.

That efficacy data, combined with the experimental drug's favorable side effect profile, has some doctors hoping that ibrutinib might one day replace the harsher chemotherapy agents that are currently the standard of care for these cancers.

"With chemotherapy, you get it for a specific period of time because patients cannot tolerate the side effects long term. This is an oral medicine that targets something the leukemia cells are dependent on but the rest of the body isn't," says Byrd.

"People can take a pill once a day and generally they tolerate it well. The side effects are much less than the chemo or other therapies that would be used in this setting."

Ibutrinib is the first agent to specifically target the BTK pathway, but it's part of a wave of new anti-cancer agents that have been developed to act as more precise, smart bomb medications that destroy just cancer cells while leaving healthy cells intact. That allows them to minimize the often intolerable side effects of harsher drugs like chemotherapy agents, which tend to wipe out both healthy and cancerous cells at once.

"In some situations there have been some medications we have tested where patients have said they would rather not be treated and pass (away) from their leukemia than go through the side effects of their medicine that is not going to cure them," says Byrd.

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Both of the clinical trials, which were sponsored by ibrutinib's developer, Pharmacyclics, involved older adults, who are most often affected by these cancers, so the researchers believe the results should be applicable to most patients diagnosed with these diseases.

The studies also suggest that patients may benefit from longer progression-free survival if they start therapy earlier in the course of their disease.

"Right now, after this drug gets approved, it will likely be used in the setting of relapse initially, but there are ongoing studies that are looking at it for initial therapy. It is something that is especially (beneficial) for elderly patients who do not tolerate chemotherapy well. This will likely replace chemotherapy," says Bryd.

The fact that even patients with the most aggressive types of CLL, which are driven by genetic mutations, responded to ibrutinib also hints that the experimental drug may become an important part of treating these cancers in coming years.

The FDA designated it as breakthrough therapy, and Pharmacyclics and Janssen, who are jointly developing the drug, plan to file a New Drug Application (NDA) with the FDA for the use of ibrutinib to treat B-cell malignancies by 2014.

This article intially published on TIME.com.

Support Groups Online

Uptodate – Patient Information Clinical Trials NIH Leukemia, Lymphoma, Myeloma BC Cancer Agency Ontario Cancer Care Leukemia and Lymphoma Society International Myeloma Foundation Association of Cancer Online Resources Myelodysplasia / Aplastic Anemia and Paroxysmal Nocturnal Hemoglobinuria Aplastic Anemia & Myelodysplasia Association of Canada (AAMAC) Marrow Forums includes support for those with AA-PNH CML Advocates Network Hemophilia Bleeding Disorders in Women Women Bleed Too The Haemophilia Society The National Hemophilia Foundation Victory For Women with Blood Disorders THE CANADIAN HEMOPHILIA SOCIETY The Haemophilia Foundation of New Zealand About Women’s Health Canadian Hemophilia Society World Federation of Hemophilia Clotting Disorders Stop the Clot The Heart.org Thrombosis Interest Group of Canada

NL Thrombosis, Blood & Immune Disorder Project March 1 Event

If you or someone you know has a blood or immune system health problem like leukemia, myeloma, lymphoma or blood clotting complications, please let them know about event at the Geo Centre. Specialists will speak about these conditions and research being done.

March 1, 2012
7 - 10 p.m.
GEO Centre
St. John’s, NL

Dr. M. Larijani will present “The human immune system; links to
leukemia and lymphoma” and

Dr. R. Chitsike will present “An overview of Venous Thromboembolic
Disease including Deep Vein Thrombosis (DVT) and Pulmonary
Embolism (PE)”

This event is open to the public.
The talks will be of interest to health-care professionals,
students, patients with their families and friends.
The lectures will discuss issues of interest for patients
living with leukemia, lymphoma, myeloma,
hypercoagulability, deep venous thrombosis
and pulmonary embolism.

Question and answer period to follow presentation.

Cash bar. Refreshments will be provided at 9 p.m.

Refreshments will be served. Everyone is welcome to attend.

Dwindling Family Size Causing Transplant Donor Shortage

Blood cancers like leukemia can be treated and possibly cured through bone marrow or stem cell transplants, but because of smaller family size, the number of sibling donors are declining, and so are the chances of patient survival. If you have leukemia for example, there is a 25% chance that a sibling will be a good enough genetic match to pursue the transplant treatment. The larger the family, the better the odds. However, family size is dwindling, and the chances of a patient getting a family match will be half of what it was only some years ago.

Transplants can save lives, though different hospitals/doctors put the success rate at anywhere between 40-75% or more. The transplant process itself is very risky for the patient, can be an 15% chance of not making it, due to infections on a wiped out immune system. Some transplants are very successful, and return many people back to their normal lives, and others have side effects (graft versus host disease), sometimes life altering follow up problems, while others just do not make it at all.

But the chances of surviving with a transplant is much greater than just from chemo and radiation alone. And, ideally the donor would be a family member, male donors for male recipients preferably too. But with smaller families comes more risks. The other hope is to receive a transplant from an outside donor, and that can save lives too. Sometimes the risks are higher for graft versus host disease complications, but other times, it works well.

So if you are ever inclined to feel like saving a life by being a possible bone marrow or stem cell donor, check out OneMatch to sign up as a donor.
p.s. Many thanks to blood donors for saving thousands of lives each year.

Genetically Modified "Serial Killer" T Cells Obliterate Tumors in Patients with Chronic Lymphocytic Leukemia,

Only a few months ago, an eye-opening breakthrough study at the University of Pennsylvania, excited the leukemia world. Here's why! With only three subjects for the study, the findings were that striking, that it has created a new hope for the treatment of CLL (chronic lymphocytic leukemia) and other cancers. The patients were in advanced stages of CLL, with few other treatment options. Researchers took patients' T-cells, then genetically modified them to attack cancer cells, and injected them back into the patients, after chemotherapy.

"Within three weeks, the tumors had been blown away, in a way that was much more violent than we ever expected," said senior author Carl June, MD, director of Translational Research and a professor of Pathology and Laboratory Medicine in the Abramson Cancer Center, who led the work. "It worked much better than we thought it would."

Patient's tumors disappeared and they went into remission, up to a year so far.

"We saw at least a 1000-fold increase in the number of modified T cells in each of the patients. Drugs don't do that," June says. "In addition to an extensive capacity for self-replication, the infused T cells are serial killers. On average, each infused T cell led to the killing of thousands of tumor cells – and overall, destroyed at least two pounds of tumor in each patient."

The research team have plans to try the same gene manipulaton on other lymphomas, and leukemias. Read the full article here

Time and more trials, and patients, will tell a fuller story, but at this point, it sounds promising for CLL patients right now, and possibly for many others in the coming years.

Launch of the NL Thrombosis, Blood and Immune Disorder Research & Education Project

The public is invited to attend this information event at the Geo Centre, St. John's, Nov. 9, 2011 at 7 pm.

Welcome to the Hemoglobin Mail!

This title began in 2002 while I was undergoing a stem cell transplant, as a treatment for the blood cancer, leukemia. It was a section of a web site where I would update family and friends on my progress and condition.

The site was a distraction of sorts and of course a way to share some information on the disease, bone marrow transplants and graft versus host disease. For a while in 2003 I kept it updated, but while life got busy in somewhat normal ways, this distraction began to lie dormant. Lately, it's been a little distracting that I have not posted much on the disease, cancer and any new and promising research. So it's about bloody time, pardon my hemoglobic pun.

Part of the motivation for turning a past hobby into a blog, is to just share any relative research news I read and hear about. Just in the last several months there have been several new promising research findings that are giving cause for a new hope for treatments. As well, here in St. John's, there will be a launch of a Thrombosis, Blood and Immune Disorder research project on Nov. 9. This blogger will talk briefly at the event, and thought that perhaps any information I write here could possibly be in some small way, encouraging to others faced with blood cancers and the side effects of treatments.

Realistically, I do not expect to write here daily, but will post whenever I learn something interesting, useful and/or positive, and will reply to any comments readers may have. For now, I say welcome, and will write more interesting posts in the days, weeks and hopefully months to come.