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Personalized Biological Testing in Psychiatry: Inevitable Reality or Impossible Dream?

By Allen Frances, MD | July 18, 2012

At next year's meeting of The International College of Neuropsychopharmacology (Collegium Internationale Neuro-Psychopharmacologicum, or CINP), the smartest people in psychiatric genetics will present their suggestions and report on progress in applying the techniques of personalized medicine as a whole new approach to psychiatric diagnosis. 

The need for out-of-the-box thinking is great. Our current diagnostic system is based on fallible and subjective clinical judgments. Progress in developing biological laboratory tests has been frustratingly slow, and except for Alzheimer disease is pretty much at a dead end. Dozens of candidate markers have been offered, but nothing ever seems to replicate.

It has become increasingly clear that each of our psychiatric diagnoses is really a heterogeneous final common pathway with dozens, perhaps hundreds, of different pathogenetic pathways. There is not one way to develop symptoms of schizophrenia or bipolar disorder or autistim or OCD. Instead, there are probably hundreds of different genotypes that can converge on the same phenotype. Explanatory mechanisms do not replicate, at least in part because patients may get their symptoms in their own very different ways.

Here is how former CINP president and conference co-host Bob Belmaker describes the issue and how the conference meant to address it: "The small effect size of antidepressants and even antipsychotics in large controlled trials has been the subject of much soul searching. These trials include very heterogeneous patient groups and the mean values may disguise huge individual variability. Personalized medicine is a new frontier of research to determine the best treatment for specific patients. CINP is organizing the first meeting on personalized medicine in psychiatry. Speakers include Tom Insel, head of the NIMH, who has made personalized medicine in psychiatry one of his top goals; Jun Wang, head of the Beijing Genomic Institute, where the government is pouring millions into drug development via the genome; and Shitij Kapur from the Maudsley Institute, who will report on individual responses in schizophrenia."

Personalized psychiatric diagnosis has great promise and may be one of the few ways out of the current impasse—the constant flow of group mean studies giving non-replicated or barely significant differences. But the path will not be easy and certainly will be slow. This is the painstakingly retail work of many professional lifetimes—akin to the steady but very slow progress in finding the heterogeneous pathways of breast cancer.

And there may be many blind alleys and false findings. If you do enough analyses you can always get positive, but meaningless, results based on chance. The statistical modeling of individual difference is still an art form in its early stages of development, and first results will require extremely cautious and skeptical interpretation.

The technique of personalized medicine will work best in situations with a favorable signal to noise ratio—conditions that have a well-demarcated and homogeneous clinical presentation with a preponderant biological contribution and patients who have a classic and severe presentation, an early onset, and many affected relatives. My guess is that the first fruits of the new approach will be in understanding severe, classic, early-onset autism, OCD, and bipolar disorder. Even the best-established contributions will probably account for just 2% to 3% of the variance—but each of these small steps will be a giant leap compared with our current stalemate in understanding the biological underpinnings of psychopathology. There will be no grand slams in this hard fought game (and no walks)—we must settle for an accumulation of singles.

More information on the CINP meeting in Jerusalem (April 21-23, 2013) can be found at www.cinp2013.com.

 

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by Ronald Pies | July 18, 2012 10:35 PM EDT

Thanks to Al Frances for an interesting and timely discussion. It's certainly the case that we have a long way to go in unraveling the pathophysiology of the most serious disorders we treat. It's also true that some so-called "lab tests"for psychiatric disorders (such as for major depression) have been over-sold and over-marketed--a topic covered in the pages of this newspaper [see Arline Kaplan's article]

But I would argue that our current state of knowledge and research is not that of a "dead end" or a "stalemate", even with respect to those elusive biomarkers and lab tests. I believe we are actually on the cusp of truly important biological findings, which, in perhaps another 5-8 years, could have real clinical utility.

To cite one brief example: a meta-analysis conducted at the University of Paris, involving 28 fMRI
or structural brain studies, found evidence of functional and anatomical alterations in bipolar disorder, in brain networks associated with the experience and regulation of emotions; e.g., increased activation in ventral limbic brain regions [Houenou et al, J Affect Disord. 2011 Aug;132(3):344-55. Epub 2011 Apr 5.]. And yet, who knew about Houenou? A careful review of the literature, in my view, will show that we know more about the pathophysiology of several neuropsychiatric diseases (including schizophrenia and major depression) than many in our own field--much less the general public--realize.

To be sure, psychiatric diagnosis--as with diagnosis in much of neurology and pain medicine--remains a clinical science and art. But we are making rapid progress in the realm of biomarkers, endophenotypes, and imaging studies.

Ron Pies MD






 
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