Most of the current treatments are approved and developed on the basis of their performance in a large population of people and each treatment is prescribed to all patients with a certain diagnosis. However, psychiatry is now developing personalized solutions for a particular patient’s needs that will become more readily available. In case of complex psychiatric disorders, the conventional “one-drug-fits-all” approach involves trial and error before appropriate treatment is found. Clinical trial data for new treatments merely show the average response of a study group. Given the considerable individual clinical and biological variation, some patients show no response whereas others show dramatic response. Although approximately 99.9% of our DNA sequence is identical, the 0.1% difference between any two individuals (except identical twins) is medically significant. Within this small percentage of difference lie the clues to hereditary susceptibility to psychiatric disorders. At the DNA level, this 0.1% difference translates into 3 million sites of genomic variation.

It is obvious that the concept of “one medicine fits all patients with the same disease” does not hold true and a more individualized approach is needed. The aim of personalized psychiatry is to match the right treatment to the right patient at the right time, and in some cases even to design the treatment for a patient according to genotype and other individual biological, psychological, or environmental characteristics.

Personalized medicine in the context of psychiatry seeks to identify environmental, biological, and clinical factors that contribute to disease vulnerability, the onset and course of mental disorders, and the predicted response to pharmacological and nonpharmacological interventions. In psychiatry, this task is complicated by the syndromic nature of diagnoses. These diagnostic categories, as represented in the Diagnostic and Statistical Manual of Mental Disorders (DSM), have been developed without a detailed understanding of underlying biological mechanisms. While they have provided the basis for the development of the science of psychiatry, they are not sufficient or reliable descriptions of an individual’s clinical presentation, response to treatment, illness, or functional trajectories, resulting in uncertainty in psychiatric diagnosis and prediction of treatment outcomes. Clinically, this may lead to a “wait and watch” approach where multiple trials of different medications with unnecessary side effects or nonefficient nonpharmacological interventions become an additional burden due to poor efficacy.

New research and clinical approaches in psychiatry have become necessary. These should aim to combine advances from clinical phenotyping, biology, neuroscience, and bioinformatic methodologies into a single but complex approach to seek better understanding of complex mental illnesses, better translate research findings into clinical practice, and stimulate reverse translation from clinical to basic science research.

By applying a personalized psychiatry approach, it is not proposed that outcomes are completely predetermined at disease onset, but that structured assessment and modeling of multivariate cross-sectional and longitudinal predictors can be used to describe the risk of specific outcome trajectories and to predict response to specific treatments. As a result, such a predictive approach could aid decision-making processes in clinical psychiatry. For this purpose, predictor variables are grouped into key psychiatric systems that can be differentiated into (a) individual clinical characteristics of a patient, including risk factors such as maternal pregnancy complications, early neurodevelopmental history, and socioeconomic status; (b) their neurocognitive, affective, and functional profile; (c) brain structure and neural function; (d) molecular profile; and (e) modulating prognostic factors such as personality, insight, and resilience. In a complex modeling approach, data from these systems are modeled to derive descriptions of illness trajectories and outcomes. In a translational next step, structured assessments feed into computerized prognostic models that are used to determine the best current treatment based on the most likely response and illness trajectory. The basic idea of these exciting developments in the field of psychiatry is conceptualized in this book.

The concept of personalized psychiatry that is presented here brings the four pillars of personalized medicine to the field of psychiatry: Prevention, Prediction, Personalization and Participation. With this approach, the fundamental questions and requirements for personalized psychiatry from a research as well as a clinical perspective will be addressed. The concept includes knowledge and extensive developments in basic science methodologies (e.g., genomics, epigenomics, transcriptomics) and neurobiological and clinical conceptual underpinnings of clinical disease relevant for personalized psychiatry. Importantly, the key principles of translation into clinical practice for the individual patient are embedded into personalized clinical trials and in complex prediction modeling. A personalized approach to mental health requires extensive developments in statistical modeling to decipher the complex interacting biological and clinical information as well as the development of a digitalized measurement-based assessment of diagnosis and treatment progression, response to treatment, and trajectories of illness. Taken together, these could transform clinical practice in psychiatry.