Downstream Polymorphisms Are Associated with Intracranial Hypertension and Statistically Interact with Polymorphisms in a Prospective Cohort of Severe Traumatic Brain Injury

Document Type

Article

Abstract

Sulfonylurea-receptor-1(SUR1) and its associated transient-receptor-potential cation channel subfamily-M (TRPM4) channel are key contributors to cerebral edema and intracranial hypertension in traumatic brain injury (TBI) and other neurological disorders. Channel inhibition by glyburide is clinically promising. (encoding SUR1) single-nucleotide polymorphisms (SNPs) are reported as predictors of raised intracranial pressure (ICP). This project evaluated whether SNPs predicted ICP and TBI outcome. DNA was extracted from 435 consecutively enrolled severe TBI patients. Without selection, all 11 SNPs available on the multiplex platform (Illumina:Human-Core-Exome v1.0) were genotyped spanning the 25 exon gene. A total of 385 patients were analyzed after quality control. Outcomes included ICP and 6 month Glasgow Outcome Scale (GOS) score. Proxy SNPs, spatial modeling, and functional predictions were determined using established software programs. rs8104571 (intron-20) and rs150391806 (exon-24) were predictors of ICP. rs8104571 heterozygotes predicted higher average ICP (β = 10.3 mm Hg,  = 0.00000029), peak ICP (β = 19.6 mm Hg,  = 0.0007), and proportion ICP >25 mm Hg (β = 0.16  = 0.004). rs150391806 heterozygotes had higher mean (β = 7.2 mm Hg,  = 0.042) and peak (β = 28.9 mm Hg,  = 0.0015) ICPs. rs8104571, rs150391806, and 34 associated proxy SNPs in linkage-disequilibrium clustered downstream. This region encodes TRPM4's channel pore and a region postulated to juxtapose SUR1 sequences encoded by an DNA segment containing previously identified relevant SNPs. There was an interaction effect on ICP between rs8104571 and a cluster of predictive SNPs (rs2237982, rs2283261, rs11024286). Although not significant in univariable or a basic multivariable model, in an expanded model additionally accounting for injury pattern, computed tomographic (CT) appearance, and intracranial hypertension, heterozygous rs8104571 was associated with favorable 6 month GOS (odds ratio [OR] = 16.7,  = 0.007951). This trend persisted in a survivor-only subcohort (OR = 20.67,  = 0.0168). In this cohort, two SNPs predicted increased ICP with large effect sizes. Both clustered downstream, spanning a region encoding the channel pore and interacting with SUR1. If validated, this may guide risk stratification and eventually inform treatment-responder classification for SUR1-TRPM4 inhibition in TBI. Larger studies are warranted.

Medical Subject Headings

Adolescent; Adult; Aged; Brain Edema (genetics); Brain Injuries, Traumatic (complications); Female; Genotype; Humans; Intracranial Hypertension (genetics); Male; Middle Aged; Polymorphism, Single Nucleotide; Prospective Studies; Sulfonylurea Receptors (genetics); TRPM Cation Channels (genetics); Young Adult

Publication Date

6-1-2019

Publication Title

Journal of neurotrauma

E-ISSN

1557-9042

Volume

36

Issue

11

First Page

1804

Last Page

1817

PubMed ID

30484364

Digital Object Identifier (DOI)

10.1089/neu.2018.6124

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