Hi Colleen,
My question, because I still do not completely understand some of this, is what is the difference between CRMS and CF? Our CF doctor said the only reason to do further testing to find my son's 2nd mutation would be to "satisfy doctors (I knew she meant one of the GI's we have seen) that want to split hairs between CRMS and CF". It was my understanding that (at least in our case) the treatments would be the same. Are kids with CRMS pancreatic insufficient? Justin is diagnosed with CF but I think she was saying (in his case) some doctors could argue for a CRMS diagnosis because the second mutation has not been found yet. We decided to wait until (for us) there is clear benefit to further testing.
Thank you in advance.
Josette
CRMS (CFTR-Related Metabolic Syndrome) is a kind of lipstick that we used to smear on a hog and take it dancing. Imagine all the red faces when two siblings with identical CFTR genetic profiles didn't both present CF? A young healthy woman follows theads trying to attach some meaning why her brother and not her is being ravaged by CF. I didn't know what CRMS meant and I made a quick study at CFF's (Cystic Fibrosis Foundation) web site.
http://www.cff.org/AboutCF/Testing/Genetics/CRMS/
I think some well intentioned person or group decided to make another stab at simplifying CF for people. Most likely some influence came from the rather embarrassed geneticists who for the umpteenth time had gotten it wrong. More kindly put, scientific questions have been answered by a new set of questions.
Wildcherry pegged it. It is the latest buzzword catch all for non homozygous presentations of CF. Genetically ideal CF is when the same CFTR mutation is inherited from both parents. (Example; genetic tests reveal two copies of DF508del (a CFTR mutation at location 508)). The reasoning is, if a person inherits the same mutation from both parents, they have CF. Technically this is an absolute. The job done by the (sodium ion) Transmembrane conductance Regulator (TR) gene in theory could be templated from either copy encoded in the halves of our DNA and we are technically
just carriers. In theory, a healthy gene works while the other fails to complete the job. Oh, if it were so simple, we are people, not pea plants!
The jury is in, having fully sequenced the TR gene, all potential permutations of the CFTR gene mutation can be read through exhaustive genetic testing. With all the new information, identical mutation pairs aren’t being discovered. Everybody bet that not finding a matched pair from an earlier genetic tests would be proven true when every mutation had been counted. What good it does over the damage is largely something to come. We, and I include myself, are being separated from the CF community over semantics. Clinical diagnosis of CF is another way of saying if it looks like a duck, quacks like duck, it is a duck for practical purposes. The difference between a healthy homozygous (containing two identical genes or gene mutations) and heterozygous (containing only one gene or one specific gene mutation) is specific in genetics and absolutely contrary in living people.
There is great importance, in fact, behind what I have been throwing matches at. As the first genetic drug just happened more because CF was a near ideal study than ending human suffering, we are a hot property right now. In order to determine what to do next, am fairly certain medicine is weeding out what has otherwise been a fairly inclusive disease. Missing the mark is too great a risk to be muddled in the sub group of clinically CF, genetically ambiguous, population.
The use of arcane terms and acronyms of acronyms is a cross science bears and shouldn't unduly inflict terms that aren't self revealing in their meaning to the broader church. The CF community ranges from people who have CF and think it is a curse from God to technologists, theoretical geneticists and very informed caregivers. I won't argue with either extreme, but I am keeping an ear open to the entire spectrum of patients, parents and practitioners. Some are being distracted by this complicated language.
CF is a little like owning an exotic pet. The curious, asking questions have driven us to learn more than we ever wanted to know about a novelty on leash. The inventions I cherish must be defined in common language if they are to have any meaning to others. Considering that dolts with degrees in this stuff are often not current on CF I am genuinely impressed at how educated and passionate CFers are. Be patient or parents, we are a studious lot. I learn something new in every single post. Sometimes what I learn is that once again, we are processing new information about CF. We are keeping current.
CRMS certainly sounds like they are pointing out GI over pulmonary patients but is purely dividing the sheep by their bleats. The wool seems to be of no importance. Don't be fleeced by any diagnostic minutia. It is neither worth the money or the misery at the moment. Someday it may serve to help manage the disease but knowing in this case is of no practical value. It won't change the course of the disease. GI problems associated with CF end up very conventionally treated. You treat gas, constipation, malabsorption, GERD (acid reflux) ad infinitum the same way whether you have CF or a just ate a bad meal.
As somebody posted recently there is more medically in common with COPD from smoking and COPD from CF than either would like. The same horrid MRSAs, yeasts, viruses and tubercleocytic (TB like) drug resistant infections. And Grandma and Grandson can kill the other with a kiss, so there goes the extended family. More to the point, the extended family I am talking about are all the microbial variety. Focus on this family for treatment.
Buy a toy badge, it is much cheaper and it come off.
LL
You know the stage where you don't care if he has it or not you just want him to get better.