Familial Combined Hyperlipidemia (FCHL) supersedes most other genetic lipid and non-lipid disorders in most of the shared scientific evidence with disease prevalence ranging from 1% to 2.5% in different parts of the globe. 1 Apparently the available data on the subjects suggests the significantly heterogeneous FCHL genetics, extremely high risk of premature coronary artery disease (CAD), hypertriglyceridemia related disorders, and relationship with other metabolic disorders like insulin resistance. 23 Unmet need must also be acknowledged on its impact on health economy in terms of this being the most frequent lipid disorder, loss of productive technical man hours, family crises emerging from premature morbidity and mortality and linkage or lead to newer metabolic disorders. 4

FCHL is not a singular entity in pathology or a monogenic genetic disorder. Molecular and genetic studies and phenotypic disease presentations have identified it as heterogeneous disease which not only vary in terms of temporo-spatial presentation clinical traits, being very pleiotropic due to probable multiple molecular triggers and the clinical appreciation variability resulting from the subtype of cholesterol surge or decline and very high prevalence in myocardial survivors. 536 All these differential presentation surrounding the singular label “FCHL” and inputs from small scale studies focusing upon few aspects of this broad-spectrum pathology makes it difficult to define the disease. 7 Nonetheless literature search converges to a few common traits which may help elucidate a criteria for nominating a person with FCHL. These criteria includes: 1- Strong family history (at least 2 members from one family), 2- Variable lipid abnormalities including combined hyperlipidemia or hypercholesterolemia or hypertriglyceridemia all shaping in different dimension over a person’s life, 3- Autosomal dominant pattern of inheritance with high penetrance, 4- Dermatological manifestations like xanthomas are rare unlike familial hypercholesterolemia and 5- Strong predisposition to early onset coronary artery disease (CAD). 8

Most primary physicians lack the knowledge and details about the gravity underlying the interpretation of a lipid profile along with being oblivious of underlying lipid pathology, so patients are dealt as per conventional wisdom with disregard to any attempt to provide the patient with complete diagnosis along with advice on family screening. Furthermore, the disease is in definitive demand of a biochemical or molecular biomarker to allow predictive screening, identifying the specific genetic defect in lipid physiology, genetic risk scoring, cascade screening of family members, preventive guidance to carriers and patients and most importantly to provide a way forward to curative medicine by gene therapy like CRISPR-Cas9 techniques. 9

This mini review attempts to segregate the molecular subtypes of FCHL, brief details of molecular pathogenesis, overlapping and contrasting evidence linking FCHL and metabolic syndrome in order to bridge the gap with some recent data and not so recent concepts about FCHL.