Rett.com » Rett Syndrome – General

RSRF and IRSA merge to form the International Rett Syndrome Foundation

Greg Long — Mon, 04 Jun 2007 18:01:17 +0000

Publisher’s note:

This is exciting news for the entire Rett Syndrome Community! As members of IRSA and long time supporters of RSRF, we look forward to being of service to this newly combined organization. Here is the press release in its entirety:

News Release:

Monday, June 04, 2007

Rett Syndrome News Release

For Immediate Release
June 4, 2007

Contact: Kathryn Kissam
804.741.3687
804.519.6231
kkissam@comcast. net

International Rett Syndrome Association and Rett Syndrome Research
Foundation Announce Merger Agreement to Form International Rett Syndrome
Foundation

New Organization to Focus on Research, Family Support, Awareness and
Advocacy

Cincinnati, Ohio – The International Rett Syndrome Association (IRSA) and
the Rett Syndrome Research Foundation (RSRF) today announced the intent to
merge their organizations to form the International Rett Syndrome Foundation
(IRSF).

“The rapid increase in scientific knowledge and pace of innovation in the
field of Rett syndrome research and treatment call for increased
coordination, increased funding and the development of a solid,
comprehensive research repository,” said Kathryn Schanen Kissam, chairman of
the board of IRSA. “By joining forces, we are able to combine the unique
expertise of IRSA and RSRF to better serve the individuals with Rett
syndrome and their families.”

“Both RSRF and IRSA have made significant contributions to the advancement
of understanding in Rett syndrome,” said Steve Gallucci, chairman of the
board of RSRF. “We are looking forward to the many opportunities that will
develop from the merging of our organizations and our mutual determination
to make a meaningful difference in the lives of those who have been touched
by Rett syndrome.”

The merger, which has been unanimously approved by both organizations’
boards, is expected to close around July 1 following the completion of
appropriate due diligence and a two-thirds vote of approval by IRSA’s
members. IRSA will declare a special membership meeting to be held at IRSA’s
offices on June 27 at 9:00 a.m.; a proxy vote will be mailed to all members
on June 4.

“I applaud the members of the governing boards of IRSA and RSRF for their
hard work and due diligence at this pivotal point in the history of Rett
syndrome. It has been my privilege to initiate the Rett syndrome movement,
and my greatest honor to see others who share the same determination and
passion join the cause,” said Kathy Hunter, president and founder of IRSA.
Hunter, who will retire from her full-time staff position with IRSA when the
merger is complete, will continue to work for the new organization in a
part-time position as Ambassador, continuing to provide ongoing support
services to families.

The core mission of IRSF will be to fund research for treatments and a cure
for Rett syndrome and to enhance the overall quality of life for those
living with Rett syndrome by providing information, programs and services.
IRSF will also place great importance on advocacy and raising awareness
about individuals with Rett syndrome so the scientific and medical
communities, along with policy-makers, educators, caregivers and the general
public, are better informed about Rett syndrome and motivated to help
research efforts.

Chuck Curley, the executive director of RSRF, will be the future executive
director of IRSF. Curley cited the critical progress made by a recent
landmark study, in which the symptoms of Rett syndrome (RTT) were reversed
in a genetic mouse model, as one example of the types of critical research
IRSF will support in the future.

“Continuing research to find a cure and treatments for Rett syndrome is
absolutely imperative, but also expensive,” Curley said. “This merger
empowers us to leverage significant revenue growth created by shared
fundraisers, collaborative minds, broader resources and combined best
practices to create one strong, unified leader in the search for a cure
while providing support services to families impacted by this disorder.”

The IRSF board of directors will be formed with six people chosen by IRSA’s
board and six chosen from RSRF’s board. Kissam will serve as chairman of
IRSF. As noted, Curley will serve as Executive Director of IRSF. Other
executive staff appointments include Monica Coenraads, who will serve as
Biomedical Research Director, and Paige Nues, who will serve as Family
Support Director.

IRSF’s executive offices will be located at the RSRF location in Cincinnati,
Ohio, with family support services operating from IRSA’s offices in Clinton,
MD. IRSF’s web site will be www.rettsyndrome. org.

About Rett Syndrome
Rett syndrome is a neurological disorder which predominately impacts girls.
While there are nearly 4,000 known cases of Rett syndrome in the United
States, the disorder is genetically linked to more widespread neurological
disorders such as autism, mental retardation and schizophrenia. Rett
symptoms begin to manifest between the first six to eighteen months of life
and eventually incapacitates the affected children so that they cannot
survive without constant care. The disorder causes seizures, respiratory and
gastrointestinal abnormalities, and a variety of muscular and motor
impairments.

About IRSA
The International Rett Syndrome Association (IRSA), founded in 1984, is the
world’s oldest and most comprehensive non-profit organization dedicated to
providing thorough and accurate information about Rett syndrome, offering
informational and educational family support, and stimulating research aimed
at finding the cause of Rett syndrome and methods for its prevention,
control and cure. The IRSA’s mission is to provide a better future for girls
with Rett syndrome. The Association has members in all 50 states and 72
foreign countries. For more information please visit www.rettsyndrome. org,
or call
1-800-818-RETT.

About RSRF
The Rett Syndrome Research Foundation was founded in late 1999 by a
passionate group of parents who were committed to funding research aimed at
finding treatments and a cure for Rett syndrome. Today RSRF is the world’s
leading private funder of Rett research. In the last five years RSRF has
funded 104 projects at premiere institutions totaling over $11 million. The
foundation has proven to be fiscally responsible by directing 97% of each
dollar donated directly to program services and was awarded Charity
Navigator’s prestigious 4-Star rating. For more information please visit
www.rsrf.org, or call
1-513-874-3020.

Rett Press: Big Bucks: Novartis focusing on rare diseases such as Rett Syndrome

Greg Long — Sat, 05 May 2007 04:21:47 +0000

Source

Forbes Magazine, May 21, 2007 edition

Summary

"For years big drugmakers ignored rare diseases. Now Novartis aims to reap billions of dollars by focusing on them. Rare diseases were long relegated to the backwaters of the drug business, targeted by tiny biotech companies, if at all, and often ignored by drug giants in their search for billion-dollar franchises. But Novartis is in pitched pursuit of some of the more obscure maladies in the world."

The article indicates that "Novartis has compounds in preclinical tests that target Rett syndrome, a rare inherited brain disorder".

Link

http://forbes.com/forbes/2007/0521/060_print.html

Rett Syndrome Fundraiser: Cape Cod Strollathon

Greg Long — Thu, 03 May 2007 02:39:01 +0000

Event

3rd Annual Cape Cod Strollathon

Date

Saturday, June 2, 2007

Location

South Yarmouth, Massachusetts, USA

Starts at Laurence MacArthur Elementary School

1175 Route 28, South Yarmouth.

Event Timetable

Registration begins at 8:45 a.m.

Strollathon begins at 10:00 a.m.

More Information

Contact Jennifer Endres at 508-394-3011 or capecodstrollathon@yahoo.com

Press Coverage

Rett Syndrome breakthrough just what the doctor ordered

http://www.townonline.com/barnstable/homepage/x301605418

Rett Syndrome Fundraiser: Elk Grove, IL April 28, 2007

Greg Long — Wed, 25 Apr 2007 19:45:15 +0000

Date

Saturday, April 28, 2007

Location

Busse Woods, Elk Grove, IL, Grove #5-16 (Enter of Higgins Road -Rt. 72 – just west of Arlington Heights Road)

Registration Information

On site registration is available. For more information please call Diane Ross at (847) 524-7540.

About This Event

From the serious runner to the recreational runner, to family members and friends of all ages the Run For Rett is an event you don’t want to miss. Make a difference in the life of those affected by Rett Syndrome; join us for the Run For Rett 5K Run/Walk & 1 Mile Fun Run.

The Cause

The mission of the International Rett Syndrome Association is to support and encourage medical research to determine the cause, treatment and cure for Rett Syndrome, and to provide informational and emotional support to families of those with Rett Syndrome.

Schedule of Events

7:00 am Race day registration and packet pick-up
8:30 am 5K Run/Walk
9:15 am 1 Mile Fun Run/Walk

Perks

ChampionChip Timing
Scenic course through the Forest Preserves.
T-shirts for the first 250 participants.
Post race activities include music, food and awards.

Packet Pick-Up
You can pick-up your packet on Saturday, April 28, 2007 at the Pre-registration Area beginning at 7:00 am.

Awards

Awards will be given to the top male and female overall finishers and to the top three male and female finishers in the designated ten year age divisions.

Timing & Results

The Run For Rett will use the ChampionChip timing system. Each participant will receive an envelope containing their timing chip. You must wear the chip on your shoe in order to be timed. No chip no time. You are responsible for returning the chip immediately after the race. Participants will be charged $30 for any lost or damaged chips. Overall results will be posted on race day. Complete results will be posted at www.chicagoaa.com

Source

www.rettsyndrome.org

An explanation for another familial case of Rett syndrome: maternal germline mosaicism

Greg Long — Mon, 23 Apr 2007 15:29:11 +0000

Abstract

Rett syndrome (RTT; OMIM#312750) is a severe neurodevelopmental disorder that affects mainly girls. It has an estimated incidence of 1:10 000–15 000 females. Mutations in the X-linked gene methyl CpG-binding protein 2 (MECP2) have been found in most patients.

The most accepted explanation for the sex bias is that the Rett mutation in sporadic cases has its origin in the paternal germline X chromosome and can thus only be transmitted to females. The majority of cases are sporadic (99.5%) but some familial cases have been described. These cases can either be explained by germline mosaicism or by asymptomatic carrier mothers with skewing of X-inactivation towards the wild-type MECP2 allele.

We describe one of the few familial cases of RTT in which a maternal germline mosaicism is the most likely explanation. The mutation p.Arg270fs (c.808delC) was identified in both a girl with classical RTT and her brother who had the severe neurological phenotype usually described in males. The mutation was absent in DNA extracted from blood of both parents.

These type of events must be taken into consideration in the genetic counselling of families after the diagnosis of a first case of RTT in a female or a MECP2 mutation in a male.

Researchers

Margarida Venâncio¹, Mónica Santos², Susana Aires Pereira³, Patrícia Maciel² and Jorge M Saraiva¹

¹Serviço de Genética Médica, Hospital Pediátrico de Coimbra, Coimbra, Portugal
²Instituto de Ciências da Vida e da Saúde (ICVS), Escola das Ciências da Saúde, Universidade do Minho, Braga, Portugal
³Serviço de Pediatria, Centro Hospitalar de Vila Nova de Gaia, Portugal

Correspondence: Professor JM Saraiva, Serviço de Genética Médica, Hospital Pediátrico de Coimbra, Av Bissaya Barreto, 3000-075 Coimbra, Portugal. Tel: +351 239 480 638; Fax: +351 239 717 216; E-mail: j.saraiva@hpc.chc.min-saude.pt

Publication

European Journal of Human Genetics advance online publication 18 April 2007; doi: 10.1038/sj.ejhg.5201835

Received 29 September 2006; Revised 8 March 2007; Accepted 17 March 2007; Published online 18 April 2007.

Abstract Source Link

http://www.nature.com/ejhg/journal/vaop/ncurrent/abs/5201835a.html

Clinical Trial: Clinical and Immunological Investigations of Subtypes of Autism

Greg Long — Sun, 15 Apr 2007 08:01:00 +0000

Purpose

The purpose of this study is to learn more about autism and its subtypes (including Rett Syndrome). Autism is a developmental disorder in which children have problems with communication and social skills and display restricted interests and repetitive behaviors.

This study has several goals. One aim is to look at types of autism that are known, such as the regressive subtype, (where skills are lost). We will explore whether there is a unique change in immune functioning related to this subtype. Another aim is to serve as one of the sites that will pilot a larger natural history study, entitled Autism Phenome Project. The goal is to further understand autism by identifying other subtypes.

We will look at several types of medical issues that may be related to autism, including immunologic problems. Children will be followed over the course of several years. We aim to capture medical problems that may be related to autism as they develop, and study outcomes in areas such as behavior and language, in order to explore known and new subtypes of autism.

Normally developing children (aged 1-6) and children with autism (age 1-6), developmental delays other than autism (age 2-6), or Rett’s disorder (age 1-4) may be eligible for this study.

Depending on each child’s study group and age, participants may undergo the following tests and procedures:

Baseline Visit

Medical and developmental history, physical examination, psychological, cognitive and medical tests to assess symptoms of autism or other developmental disorders, photographs of the child’s face, collection of hair, urine and baby teeth samples. If available, hair samples from the baby’s first haircut and from the biological mother’s hair are also collected.
Overnight electroencephalogram (EEG; for children autism developmental delays and Rett Syndrome): A special cap with electrodes is placed on the child’s head to measure brain waves (brain electrical activity) while the child sleeps in the hospital overnight. Healthy volunteers do not undergo this procedure.
Magnetic resonance imaging (MRI) scan: The child stays in the scanner, lying still for 10 to 15 minutes at a time. Since it may be difficult for the child to lie still, the test may be scheduled for a time when the child is likely to be sleepy, or the child may be sedated.
Lumbar puncture (for some children in the autism, developmental delay and Rett Syndrome groups). This test may be done under sedation.

Follow-Up Visits

Follow-up visits are scheduled at different intervals, depending on study group, age and aspect of the study the child is enrolled in. The visits include a short interview session with the child’s caregiver and assessment of the child’s development and behavior. Some of the assessment measures used during the baseline examination are repeated, including symptoms ratings, behavioral tests and a blood test. For some children, the final visit will include repeats of the medical procedures.

Study Type: Observational
Study Design: Natural History

Official Title: Clinical and Immunological Investigations of Subtypes of Autism

Further study details as provided by National Institutes of Health Clinical Center (CC):

Expected Total Enrollment: 250

Study start: February 2006

The current investigation will focus on the interrelationship between regression in autism and immune dysfunction. We propose to conduct a longitudinal natural history study that will result in a sample of 50 children with autism and strictly defined regression, 50 children with autism and no history of regression, 50 typically developing children, and 25 children who meet criteria for Rett’s Disorder (a genetic disorder in which children have autistic features with clear regression). Subjects will be 12-48 months of age at study entry in order to capture regression as close to its onset as possible. Systematic prospective evaluations will be utilized in order to provide validation to the phenomenon of regression in autism, determine diagnostic and functional outcomes, and evaluate behavioral, medical and immunologic functioning. These evaluations will include comprehensive medical history, behavioral assessment, physical and neurologic examination, sleep EEG, structural MRI, blood work for laboratory assays, and for some children, lumbar puncture. In an investigation of potential immunologic abnormalities and associated neuroinflammation, repeated assessments are necessary to determine whether both behavioral and/or immunologic parameters are due to state versus trait alterations: elements of these assessments will be conducted every 6 to 12 months, depending on the child’s age.

Our objective is to determine if there is a unique alteration in immune function among autistic children with a regressive clinical course. Our primary hypothesis is that at least some children with regressive autism will have abnormalities in immune function. These abnormalities will not be found among autistic children without a regressive course nor will they be found among children without an autistic spectrum disorder. Our specific aims are:

Specific Aim #1: To characterize and validate the regressive phenotype in children with autism.

Working hypothesis: Children with the diagnosis of autism who had a regressive clinical course can be reliably distinguished from children with non-regressive autism, Rett’s Disorder and healthy children. When compared to children with non-regressive autism, the history of children in the regressive group will consist of similar or higher skill levels prior to regression, and lower skill levels following regression.

Specific Aim #2: To characterize the immune response in children with autism.

Working Hypothesis 2a: Distinct immunologic responses and cytokine abnormalities will be evident in children in the regressive autism sample, but not in the non-regressive autism, Rett’s Disorder, or typically developing samples.

Working Hypothesis 2b: MRI scans will reveal regional neuroinflammation among children in the regressive autism sample, but not in the non-regressive autism, Rett’s Disorder, or typically developing samples.

Specific Aim #3: To identify neurobiologic markers for autism through the techniques of metabolomics, proteomics and genomics (e.g. gene expression profiles).

Working hypothesis: These neurobiologic markers will reliably differentiate between regressive autism, non-regressive autism, Rett’s Disorder, and typically developing children.

In addition, although progress has been made in identifying children affected by autism, little attention has been paid to the different manifestations of autism (or autisms). As has been demonstrated in "diabetes" and "cancer", it is expected that the differences between individuals with autism may be as informative as their behavioral similarities. Complementing this study that investigates one possible subtype (regression), we propose to pilot a phenomenologic investigation to identify other biological and behavioral subgroups of autistic individuals, in order to facilitate investigations of etiology, pathophysiology, treatment and prevention. The present investigation thus includes a pilot study to evaluate feasibility of conducting a large-scale, multi-site longitudinal investigation of 1,800 children (600 children with autism, 600 healthy controls, and 600 children with developmental delays). The protocol has been approved by the UC-Davis IRB (see attachments) and the study is currently underway at the M.I.N.D. Institute in Sacramento, California. NIMH is an ideal second site for the protocol, because of the overlap between the design of this regression study with their Autism Phenome Project. Children participating in 06-M-0102 will be invited to participate in this study; if interested, their data will be entered into the Phenome study. The age at study entry for the Phenome study (2 – 6 years) is slightly older than the original regression study, so we will recruit up to 25 children with autism and 25 age-/sex-matched healthy controls to this investigation. In addition, as many as 25 children (ages 2 – 6 years) with developmental delays (without autism) will be recruited as contrast subjects.

Eligibility

Ages Eligible for Study: 1 Year - 6 Years, Genders Eligible for Study: Both

Accepts Healthy Volunteers

Inclusion Criteria

The sample at study endpoint will contain 50 children diagnosed with idiopathic autism and regression (AUT-R), 50 children diagnosed with idiopathic autism (and no history of regression; AUT-NR), 25 children with Rett’s Disorder (RTT) and 50 typically developing children (TYP), matched on ethnicity, sex, chronological age and daycare enrollment. Matching for daycare setting (home versus setting with other children) will be attempted due to the potentially greater immunologic challenge experienced by children in daycare settings. The age range of all groups will be between 12 and 48 months at first visit. We will over-recruit for children in the 12-36 month age range, in order to maximize participants of the age when regression associated with the autism diagnosis is most likely.

The Phenome Project Pilot will also enroll an additional 25 children with autism and 25 age-/sex-matched healthy controls, aged 2-6. In addition, as many as 25 children (ages 2 – 6 years) with developmental delays (without autism) will be recruited as contrast subjects.

Regression will be defined as:

Language loss: Loss of at least 3 spontaneously meaningful words (excluding mama or dada) used for at least a month, and lost for at least a month.

AND/OR

Nonverbal communication/social loss: Loss of more than one nonverbal communicative behavior (e.g. gestures, joint attention, eye contact, imagination, pretend play, sharing, showing, watching children, orienting to name, social smiling, social games, spontaneous imitation of actions, response to social overtures).

Autism groups (AUT-R & AUT-NR): Children with a diagnosis of autism or referral from professional with concerns of a diagnosis of autism will be evaluated with the ADI-R and ADOS. Those meeting research criteria for autism will be included.

Although there is overlap in the age period for regression specified in this protocol (regression between 15-30 months) and that described for childhood disintegrative disorder (CDD) (the DSM-IV criteria for CDD indicate apparently normal development for the first 2 years after birth), the criteria for CDD also indicate a diagnosis can only be made if symptoms are not better accounted for by another pervasive developmental disorder such as autism. Symptoms of CDD that separate it from autism include loss of acquired skills in areas such as motor skills and bowel or bladder control, while the focus of the current study is on regression in core symptoms of autism (i.e. socio-communicative skills). Thus, the current protocol will include children with regression over 2 who meet criteria for autism, but not those who only meet criteria for CDD.

Rett’s Disorder group (RTT): Positive genetic screen for MeCP2 genetic mutation.

Typically Developing control group (TYP): No diagnosis of developmental delay and no first-degree relatives with history of developmental problems.

Developmental Delay group (DD): Developmental scores (Performance Quotient and Verbal Quotient) greater than 1.5 standard deviations below mean on Mullens Scale of Early Learning

Exclusion Criteria:

Known genetic defect (e.g. Fragile X, Down Syndrome, Tuberous Sclerosis, etc.). The Developmentally Delayed group may include children with such defects.
Significant prematurity at birth (less than 32 weeks gestation); birthweight significantly below normal for gestational age (SGA- small for gestational age); or diagnosis of cerebral palsy.
If behavioral management issues (e.g. self-injury, aggressiveness) are severe to the extent that the screening protocol was aborted.

Location and Contact Information

Please refer to this study by ClinicalTrials.gov identifier NCT00298246

Patient Recruitment and Public Liaison Office (800) 411-1222 prpl@mail.cc.nih.gov
TTY 1-866-411-1010

Locations: United States

California
University of California, Davis, Davis, California, 95616

District of Columbia
Childrens National Medical Center, Washington, District of Columbia

Maryland
National Institutes of Health Clinical Center, 9000 Rockville Pike, Bethesda, Maryland

Johns Hopkins University, Baltimore, Maryland

Tennessee
Vanderbilt University, Nashville, Tennessee

More Information

Study ID Numbers: 060102; 06-M-0102
Last Updated: March 9, 2007
Record first received: March 1, 2006
ClinicalTrials.gov Identifier: NCT00298246
Health Authority: United States: Federal Government

Ten years of searching and learning

Greg Long — Fri, 13 Apr 2007 10:42:23 +0000

I first learned about Rett syndrome in 1997. A devoted physical therapist mentioned her suspicion that our daughter had Rett syndrome during a therapy session. The disorder seemed to perfectly describe my two year-old daughter’s apparently imperfect health condition. The best doctors at one of America’s finest University hospitals missed the diagnosis altogether because they simply had never heard of Rett Syndrome in 1997. The first night I learned about Rett syndrome I searched online for more than seven hours.

In my role as a Rett Dad I have spent countless hours surfing the web looking for the latest insight and information about how to make a difference in her life. That first night after meeting with the therapist I “met” people on-line whom I continue to share close ties with even today. There are many people in the Rett syndrome community with much more expertise and experience than me. Those newer to Rett syndrome also have a great deal of wisdom and experience to share. Some people have devoted the majority of their personal and professional lives to the same mission of this magazine – to make a difference in the lives of those with Rett Syndrome and those who love them, befriend them, treat them, and otherwise serve them. We believe that important knowledge and expertise about Rett syndrome should be freely shared. Rett.com and other online resources were developed with that purpose in mind.

If you would like to share your personal or professional expertise, insight, challenges, solutions, stories, and recommendations as a guest columnist or researcher, please contact us at the link to the left. We also appreciate your patience and feedback as we work to build this online magazine into a valuable resource for all in the Rett syndrome community. If you find a dead link, please let us know. If we have erred or offended you in any way, please give us a chance to rectify our mistakes. Stay tuned.