Genetic variants in TREM2 are strongly associated with Alzheimer’s disease (AD) risk but alternative splicing in TREM2 transcripts has not been comprehensively described.
Objective:
Recognizing that alternative splice variants can result in reduced gene expression and/or altered function, we sought to fully characterize splice variation in TREM2.
Methods:
Human anterior cingulate autopsy tissue from 61 donors was used for end-point and quantitative PCR and western blotting to identify and quantify novel TREM2 isoforms.
Results:
In addition to previously described transcripts lacking exon 3 or exon 4, or retaining part of intron 3, we identified novel isoforms lacking exon 2, along with isoforms lacking multiple exons. Isoforms lacking exon 2 were predominant at approximately 10% of TREM2 mRNA in the brain. Expression of TREM2 and frequency of exon 2 skipping did not differ between AD samples and non-AD controls (p = 0.1268 and p = 0.4909, respectively). Further, these novel splice isoforms were also observed across multiple tissues with similar frequency (range 5.3 –13.0%). We found that the exon 2 skipped isoform D2-TREM2 is translated to protein and localizes similarly to full-length TREM2 protein, that both proteins are primarily retained in the Golgi complex, and that D2-TREM2 is expressed in AD and non-AD brain.
Conclusion:
Since the TREM2 ligand binding domain is encoded by exon 2, and skipping this exon retains reading frame while conserving localization, we hypothesize that D2-TREM2 acts as an inhibitor of TREM2 and targeting TREM2 splicing may be a novel therapeutic pathway for AD.
JonssonT, StefanssonH, SteinbergS, JonsdottirI, JonssonPV, SnaedalJ, BjornssonS, HuttenlocherJ, LeveyAI, LahJJ, RujescuD, HampelH, GieglingI, AndreassenOA, EngedalK, UlsteinI, DjurovicS, Ibrahim-VerbaasC, HofmanA, IkramMA, Van DuijnCM, ThorsteinsdottirU, KongA, StefanssonK (2013) Variant of TREM2 associated with the risk of Alzheimer’s disease. N Engl J Med368, 107–116.
2.
GuerreiroR, WojtasA, BrasJ, CarrasquilloM, RogaevaE, MajounieE, CruchagaC, SassiC, KauweJS, YounkinS, HazratiL, CollingeJ, PocockJ, LashleyT, WilliamsJ, LambertJC, AmouyelP, GoateA, RademakersR, MorganK, PowellJ, St George-HyslopP, SingletonA, HardyJAlzheimer Genetic Analysis Group (2013) TREM2 variants in Alzheimer’s disease. N Engl J Med368, 117–127.
3.
PalonevaJ, ManninenT, ChristmanG, HovanesK, MandelinJ, AdolfssonR, BianchinM, BirdT, MirandaR, SalmaggiA, TranebjærgL, KonttinenY, PeltonenL (2002) Mutations in two genes encoding different subunits of a receptor signaling complex result in an identical disease phenotype. Am J Hum Genet71, 656–662.
4.
KunkleBW, Grenier-BoleyB, SimsR, BisJC, DamotteV, NajAC, BolandA, VronskayaM, van der LeeSJ, Amlie-WolfA, et al. (2019) Genetic meta-analysis of diagnosed Alzheimer’s disease identifies new risk loci and implicates Abeta, tau, immunity and lipid processing. Nat Genet51, 414–430.
5.
LambertJC, Ibrahim-VerbaasCA, HaroldD, NajAC, SimsR, BellenguezC, DeStafanoAL, BisJC, BeechamGW, Grenier-BoleyB, et al. (2013) Meta-analysis of 74,046 individuals identifies 11 new susceptibility loci for Alzheimer’s disease. Nat Genet45, 1452–1458.
DeanHB, RobersonED, SongY (2019) Neurodegenerative disease–associated variants in TREM2 destabilize the apical ligand-binding region of the immunoglobulin domain. Front Neurol10, 1252.
9.
GratuzeM, LeynsCEG, SauerbeckAD, St-PierreM-K, XiongM, KimN, SerranoJR, TremblayM-È, KummerTT, ColonnaM, UlrichJD, HoltzmanDM (2020) Impact of TREM2R47H variant on tau pathology–induced gliosis and neurodegeneration. J Clin Invest130, 4954–4968.
10.
PiersTM, CoskerK, MallachA, JohnsonGT, GuerreiroR, HardyJ, PocockJM (2020) A locked immunometabolic switch underlies TREM2 R47H loss of function in human iPSC-derived microglia. FASEB J34, 2436–2450.
11.
CoskerK, MallachA, LimayeJ, PiersTM, StaddonJ, NeameSJ, HardyJ, PocockJM (2021) Microglial signalling pathway deficits associated with the patient derived R47H TREM2 variants linked to AD indicate inability to activate inflammasome. Sci Rep11, 13316.
12.
AtagiY, LiuC-C, PainterMM, ChenX-F, VerbeeckC, ZhengH, LiX, RademakersR, KangSS, XuH, YounkinS, DasP, FryerJD, BuG (2015) Apolipoprotein E is a ligand for triggering receptor expressed on myeloid cells 2 (TREM2). J Biol Chem290, 26043–26050.
13.
ZhaoY, WuX, LiX, JiangL-L, GuiX, LiuY, SunY, ZhuB, Piña-CrespoJC, ZhangM, ZhangN, ChenX, BuG, AnZ, HuangTY, XuH (2018) TREM2 is a receptor for β-amyloid that mediates microglial function. Neuron97, 1023–1031.e1027.
Del-AguilaJL, BenitezBA, LiZ, DubeU, MihindukulasuriyaKA, BuddeJP, FariasFHG, FernándezMV, IbanezL, JiangS, PerrinRJ, CairnsNJ, MorrisJC, HarariO, CruchagaC (2019) TREM2 brain transcript-specific studies in AD and TREM2 mutation carriers. Mol Neurodegener14, 18.
21.
YanaizuM, SakaiK, TosakiY, KinoY, SatohJ-i (2018) Small nuclear RNA-mediated modulation of splicing reveals a therapeutic strategy for a TREM2 mutation and its post-transcriptional regulation. Sci Rep8, 6937.
22.
NumasawaY, YamauraC, IshiharaS, ShintaniS, YamazakiM, TabunokiH, SatohJI (2011) Nasu-Hakola disease with a splicing mutation of TREM2 in a Japanese family. Eur J Neurol18, 1179–1183.
23.
FinkelRS, MercuriE, DarrasBT, ConnollyAM, KuntzNL, KirschnerJ, ChiribogaCA, SaitoK, ServaisL, TizzanoE, TopalogluH, TuliniusM, MontesJ, GlanzmanAM, BishopK, ZhongZJ, GheuensS, BennettCF, SchneiderE, FarwellW, De VivoDC (2017) Nusinersen versus sham control in infantile-onset spinal muscular atrophy. N Engl J Med377, 1723–1732.
24.
KiianitsaK, KurtzI, BeemanN, MatsushitaM, ChienW-M, RaskindWH, KorvatskaO (2021) Novel TREM2 splicing isoform that lacks the V-set immunoglobulin domain is abundant in the human brain. J Leukoc Biol110, 829–837.
25.
ZouF, GopalrajRK, LokJ, ZhuH, LingIF, SimpsonJF, TuckerHM, KellyJF, YounkinSG, DicksonDW, PetersenRC, Graff-RadfordNR, BennettDA, CrookJE, YounkinSG, EstusS (2007) Sex-dependent association of a common low-density lipoprotein receptor polymorphism with RNA splicing efficiency in the brain and Alzheimer’s disease. Hum Mol Genet17, 929–935.
26.
BurchettME, LingIF, EstusS (2011) FBN1 isoform expression varies in a tissue and development-specific fashion. Biochem Biophys Res Commun411, 323–328.
27.
SessaG, PodiniP, MarianiM, MeroniA, SpreaficoR, SinigagliaF, ColonnaM, PaninaP, MeldolesiJ (2004) Distribution and signaling of TREM2/DAP12, the receptor system mutated in human polycystic lipomembraneous osteodysplasia with sclerosing leukoencephalopathy dementia. Eur J Neurosci20, 2617–2628.
28.
PradaI, OnganiaGN, BuonsantiC, Panina-BordignonP, MeldolesiJ (2006) Triggering receptor expressed in myeloid cells 2 (TREM2) trafficking in microglial cells: Continuous shuttling to and from the plasma membrane regulated by cell stimulation. Neuroscience140, 1139–1148.
29.
HanS, NaY, KohI, NhoK, LeeY (2021) Alternative splicing regulation of low-frequency genetic variants in exon 2 of TREM2 in Alzheimer’s disease by splicing-based aggregation. Int J Mol Sci22, 9865.
30.
PengQ, MalhotraS, TorchiaJA, KerrWG, CoggeshallKM, HumphreyMB (2010) TREM2- and DAP12-dependent activation of PI3K requires DAP10 and is inhibited by SHIP1. Sci Signal3, ra38.
31.
SchlepckowK, KleinbergerG, FukumoriA, FeederleR, LichtenthalerSF, SteinerH, HaassC (2017) An Alzheimer-associated TREM2 variant occurs at the ADAM cleavage site and affects shedding and phagocytic function. EMBO Mol Med9, 1356–1365.
32.
ZhongL, ChenX-F, ZhangZ-L, WangZ, ShiX-Z, XuK, ZhangY-W, XuH, BuG (2015) DAP12 stabilizes the C-terminal fragment of the triggering receptor expressed on myeloid cells-2 (TREM2) and protects against LPS-induced pro-inflammatory response. J Biol Chem290, 15866–15877.
33.
KarchCM, GoateAM (2015) Alzheimer’s disease risk genes and mechanisms of disease pathogenesis. Biol Psychiatry77, 43–51.
34.
EstusS, ShawBC, DevanneyN, KatsumataY, PressEE, FardoDW (2019) Evaluation of CD33 as a genetic risk factor for Alzheimer’s disease. Acta Neuropathol138, 187–199.
35.
BhattacherjeeA, JungSJ, HoM, Eskandari-SedighiG, St.LaurentCD, McCordKA, BainsA, GauravS, SarkarSS, PlemelJ, MacauleyMS (2021) The CD33 short isoform is a gain-of-function variant that enhances Aβ1-42 phagocytosis in microglia. Mol Neurodegener16, 19.
36.
WiβfeldJ, MathewsM, MossadO, PicardiP, CintiA, RedaelliL, PradierL, BrüstleO, NeumannH (2021) Reporter cell assay for human CD33 validated by specific antibodies and human iPSC-derived microglia. Sci Rep11, 13492.
37.
WiβfeldJ, NozakiI, MathewsM, RaschkaT, EbelingC, HornungV, BrustleO, NeumannH (2021) Deletion of Alzheimer’s disease-associated CD33 results in an inflammatory human microglia phenotype. Glia69, 1393–1412.
38.
EwersM, BiecheleG, Suárez-CalvetM, SacherC, BlumeT, Morenas-RodriguezE, DemingY, PiccioL, CruchagaC, KleinbergerG, ShawL, TrojanowskiJQ, HermsJ, DichgansM, BrendelM, HaassC, FranzmeierN (2020) Higher CSF sTREM2 and microglia activation are associated with slower rates of beta-amyloid accumulation. . EMBO Mol Med12.
