Restricted accessResearch articleFirst published online 2024-05-07
The Use of Zebrafish in Transcriptome Analysis of the Early Effects of Mutations Causing Early Onset Familial Alzheimer’s Disease and Other Inherited Neurodegenerative Conditions
The degree to which non-human animals can be used to model Alzheimer’s disease is a contentious issue, particularly as there is still widespread disagreement regarding the pathogenesis of this neurodegenerative dementia. The currently popular transgenic models are based on artificial expression of genes mutated in early onset forms of familial Alzheimer’s disease (EOfAD). Uncertainty regarding the veracity of these models led us to focus on heterozygous, single mutations of endogenous genes (knock-in models) as these most closely resemble the genetic state of humans with EOfAD, and so incorporate the fewest assumptions regarding pathological mechanism. We have generated a number of lines of zebrafish bearing EOfAD-like and non-EOfAD-like mutations in genes equivalent to human PSEN1, PSEN2, and SORL1. To analyze the young adult brain transcriptomes of these mutants, we exploited the ability of zebrafish to produce very large families of simultaneous siblings composed of a variety of genotypes and raised in a uniform environment. This “intra-family” analysis strategy greatly reduced genetic and environmental “noise” thereby allowing detection of subtle changes in gene sets after bulk RNA sequencing of entire brains. Changes to oxidative phosphorylation were predicted for all EOfAD-like mutations in the three genes studied. Here we describe some of the analytical lessons learned in our program combining zebrafish genome editing with transcriptomics to understand the molecular pathologies of neurodegenerative disease.
NakanoY, KondohG, KudoT, ImaizumiK, KatoM, MiyazakiJI, TohyamaM, TakedaJ, TakedaM (1999) Accumulation of murine amyloidbeta42 in a gene-dosage-dependent manner in PS1 ‘knock-in’ mice. Eur J Neurosci11, 2577–2581.
4.
McKeanNE, HandleyRR, SnellRG (2021) A review of the current mammalian models of Alzheimer’s disease and challenges that need to be overcome. Int J Mol Sci22, 13168.
5.
FoleyAM, AmmarZM, LeeRH, MitchellCS (2015) Systematic review of the relationship between amyloid-beta levels and measures of transgenic mouse cognitive deficit in Alzheimer’s disease. J Alzheimers Dis44, 787–795.
6.
HargisKE, BlalockEM (2017) Transcriptional signatures of brain aging and Alzheimer’s disease: What are our rodent models telling us?Behav Brain Res322, 311–328.
7.
SaitoT, MatsubaY, MihiraN, TakanoJ, NilssonP, ItoharaS, IwataN, SaidoTC (2014) Single App knock-in mouse models of Alzheimer’s disease. Nat Neurosci17, 661–663.
8.
PangK, JiangR, ZhangW, YangZ, LiL-L, ShimozawaM, TambaroS, MayerJ, ZhangB, LiM, WangJ, LiuH, YangA, ChenX, LiuJ, WinbladB, HanH, JiangT, WangW, NilssonP, GuoW, LuB (2022) An App knock-in rat model for Alzheimer’s disease exhibiting Aβ and tau pathologies, neuronal death and cognitive impairments. Cell Res32, 157–175.
9.
BarthelsonK, NewmanM, LardelliM (2022) Brain transcriptomes of zebrafish and mouse Alzheimer’s disease knock-in models imply early disrupted energy metabolism. Dis Model Mech15, dmm049187.
10.
ParkH, ChoB, KimH, SaitoT, SaidoTC, WonKJ, KimJ (2023) Single-cell RNA-sequencing identifies disease-associated oligodendrocytes in male APP NL-G-F and 5XFAD mice. Nat Commun14, 802.
11.
KhalilAM (2020) The genome editing revolution: review. J Genet Eng Biotechnol18, 68.
12.
DoetschmanT, GreggRG, MaedaN, HooperML, MeltonDW, ThompsonS, SmithiesO (1987) Targetted correction of a mutant HPRT gene in mouse embryonic stem cells. Nature330, 576–578.
13.
ThomasKR, CapecchiMR (1987) Site-directed mutagenesis by gene targeting in mouse embryo-derived stem cells. Cell51, 503–512.
14.
OblakAL, FornerS, TerritoPR, SasnerM, CarterGW, HowellGR, Sukoff-RizzoSJ, LogsdonBA, MangraviteLM, MortazaviA, Baglietto-VargasD, GreenKN, MacGregorGR, WoodMA, TennerAJ, LaFerlaFM, LambBT, and The MODEL-AD; Consortium (2020) Model organism development and evaluation for late-onset Alzheimer’s disease: MODEL-AD. Alzheimers Dement (N Y)6, e12110.
15.
GemberlingM, BaileyTJ, HydeDR, PossKD (2013) The zebrafish as a model for complex tissue regeneration. Trends Genet29, 611–620.
16.
HinN, NewmanM, KaslinJ, DouekAM, LumsdenA, NikSHM, DongY, ZhouXF, Manucat-TanNB, LudingtonA, AdelsonDL, PedersonS, LardelliM (2020) Accelerated brain aging towards transcriptional inversion in a zebrafish model of the K115fs mutation of human PSEN2. PLoS One15, e0227258.
17.
ChiaK, KlingseisenA, SiegerD, PrillerJ (2022) Zebrafish as a model organism for neurodegenerative disease. Front Mol Neurosci15, 940484.
18.
MusaA, LehrachH, RussoVA (2001) Distinct expression patterns of two zebrafish homologues of the human APP gene during embryonic development. Dev Genes Evol211, 563–567.
19.
OtisJP, ZeituniEM, ThiererJH, AndersonJL, BrownAC, BoehmED, CerchioneDM, CeasrineAM, Avraham-DavidiI, TempelhofH, YanivK, FarberSA (2015) Zebrafish as a model for apolipoprotein biology: comprehensive expression analysis and a role for ApoA-IV in regulating food intake. Dis Model Mech8, 295–309.
20.
MooreDB, GillentineMA, BotezatuNM, WilsonKA, BensonAE, LangelandJA (2014) Asynchronous evolutionary origins of Abeta and BACE1. Mol Biol Evol31, 696–702.
BhattaraiP, ThomasAK, CosacakMI, PapadimitriouC, MashkaryanV, ZhangY, KizilC (2017) Modeling amyloid-beta42 toxicity and neurodegeneration in adult zebrafish brain. J Vis Exp, 56014.
23.
CosacakMI, BhattaraiP, ReinhardtS, PetzoldA, DahlA, ZhangY, KizilC (2019) Single-cell transcriptomics analyses of neural stem cell heterogeneity and contextual plasticity in a zebrafish brain model of amyloid toxicitye. Cell Rep27, 1307–1318e1303.
24.
SharmanMJ, Moussavi NikSH, ChenMM, OngD, WijayaL, LawsSM, TaddeiK, NewmanM, LardelliM, MartinsRN, VerdileG (2013) The guinea pig as a model for sporadic Alzheimer’s disease (AD): the impact of cholesterol intake on expression of AD-related genes. PLoS One8, e66235.
25.
Moussavi NikSH, NewmanM, WilsonL, EbrahimieE, WellsS, MusgraveI, VerdileG, MartinsRN, LardelliM (2015) Alzheimer’s disease-related peptide PS2V plays ancient, conserved roles in suppression of the unfolded protein response under hypoxia and stimulation of gamma-secretase activity. Hum Mol Genet24, 3662–3678.
26.
SatoN, ImaizumiK, ManabeT, TaniguchiM, HitomiJ, KatayamaT, YonedaT, MoriharaT, YasudaY, TakagiT, KudoT, TsudaT, ItoyamaY, MakifuchiT, FraserPE, St George-Hyslop P, TohyamaM (2001) Increased production of beta-amyloid and vulnerability to endoplasmic reticulum stress by an aberrant spliced form of presenilin 2. J Biol Chem276, 2108–2114.
27.
KatayamaT, ImaizumiK, ManabeT, HitomiJ, KudoT, TohyamaM (2004) Induction of neuronal death by ER stress in Alzheimer’s disease. J Chem Neuroanat28, 67–78.
28.
KumarS, HedgesSB (1998) A molecular timescale for vertebrate evolution. Nature392, 917–920.
29.
CrowM, SureshH, LeeJ, GillisJ (2022) Coexpression reveals conserved gene programs that co-vary with cell type across kingdoms. Nucleic Acids Res50, 4302–4314.
30.
WileyDS, RedfieldSE, ZonLI (2017) Chemical screening in zebrafish for novel biological and therapeutic discovery. Methods Cell Biol138, 651–679.
31.
AdattoI, LawrenceC, KrugL, ZonLI (2022) The effects of intensive feeding on reproductive performance in laboratory zebrafish (Danio rerio). PLoS One17, e0278302.
32.
BarthelsonK, PedersonSM, NewmanM, LardelliM (2021) Brain transcriptome analysis of a protein-truncating mutation in sortilin-related receptor 1 associated with early-onset familial Alzheimer’s disease indicates early effects on mitochondrial and ribosome function. J Alzheimers Dis79, 1105–1119.
33.
BarthelsonK, DongY, NewmanM, LardelliM (2021) PRESENILIN 1 mutations causing early-onset familial Alzheimer’s disease or familial acne inversa differ in their effects on genes facilitating energy metabolism and signal transduction. J Alzheimers Dis82, 327–347.
IshikawaA, PiaoYS, MiyashitaA, KuwanoR, OnoderaO, OhtakeH, SuzukiM, NishizawaM, TakahashiH (2005) A mutant PSEN1 causes dementia with Lewy bodies and variant Alzheimer’s disease. Ann Neurol57, 429–434.
36.
BarthelsonK, PedersonSM, NewmanM, JiangH, LardelliM (2021) In-frame and frameshift mutations in zebrafish presenilin 2 affect different cellular functions in young adult brains. J Alzheimers Dis Rep5, 395–404.
37.
BarthelsonK, PedersonSM, NewmanM, LardelliM (2020) Brain transcriptome analysis reveals subtle effects on mitochondrial function and iron homeostasis of mutations in the SORL1 gene implicated in early onset familial Alzheimer’s disease. Mol Brain13, 142.
38.
NewmanM, HinN, PedersonS, LardelliM (2019) Brain transcriptome analysis of a familial Alzheimer’s disease-like mutation in the zebrafish presenilin 1 gene implies effects on energy production. Mol Brain12, 43.
39.
JiangH, NewmanM, LardelliM (2018) The zebrafish orthologue of familial Alzheimer’s disease gene PRESENILIN 2 is required for normal adult melanotic skin pigmentation. PLoS One13, e0206155.
40.
JiangH, PedersonSM, NewmanM, DongY, BarthelsonK, LardelliM (2020) Transcriptome analysis indicates dominant effects on ribosome and mitochondrial function of a premature termination codon mutation in the zebrafish gene psen2. PLoS One15, e0232559.
41.
NooriA, MezliniAM, HymanBT, Serrano-PozoA, DasS (2021) Systematic review and meta-analysis of human transcriptomics reveals neuroinflammation, deficient energy metabolism, and proteostasis failure across neurodegeneration. Neurobiol Dis149, 105225.
42.
YuL, JinJ, XuY, ZhuX (2022) Aberrant energy metabolism in Alzheimer’s disease. J Transl Int Med10, 197–206.
43.
OzgenS, KrigmanJ, ZhangR, SunN (2022) Significance of mitochondrial activity in neurogenesis and neurodegenerative diseases. Neural Regen Res17, 741–747.
44.
YambireKF, RostoskyC, WatanabeT, Pacheu-GrauD, Torres-OdioS, Sanchez-GuerreroA, SenderovichO, Meyron-HoltzEG, MilosevicI, FrahmJ, WestAP, RaimundoN (2019) Impaired lysosomal acidification triggers iron deficiency and inflammation in vivo. Elife8, e51031.
45.
JiangY, SatoY, ImE, BergM, BordiM, DarjiS, KumarA, MohanPS, BandyopadhyayU, DiazA, CuervoAM, NixonRA (2019) Lysosomal dysfunction in Down syndrome is APP-dependent and mediated by APP-betaCTF (C99). J Neurosci39, 5255–5268.
46.
LeeJH, YuWH, KumarA, LeeS, MohanPS, PeterhoffCM, WolfeDM, Martinez-VicenteM, MasseyAC, SovakG, UchiyamaY, WestawayD, CuervoAM, NixonRA (2010) Lysosomal proteolysis and autophagy require presenilin 1 and are disrupted by Alzheimer-related PS1 mutations. Cell141, 1146–1158.
47.
PrasadH, RaoR (2018) Amyloid clearance defect in ApoE4 astrocytes is reversed by epigenetic correction of endosomal pH. Proc Natl Acad Sci U S A115, E6640–E6649.
48.
KennedyMC, Mende-MuellerL, BlondinGA, BeinertH (1992) Purification and characterization of cytosolic aconitase from beef liver and its relationship to the iron-responsive element binding protein. Proc Natl Acad Sci U S A89, 11730–11734.
49.
TerziEM, SviderskiyVO, AlvarezSW, WhitenGC, PossematoR (2021) Iron-sulfur cluster deficiency can be sensed by IRP2 and regulates iron homeostasis and sensitivity to ferroptosis independent of IRP1 and FBXL5. Sci Adv7, eabg4302.
50.
HinN, NewmanM, PedersonS, LardelliM (2021) Iron responsive element-mediated responses to iron dyshomeostasis in Alzheimer’s disease. J Alzheimers Dis84, 1597–1630.
WilkinsonB (1951) A statistical consideration in psychological research. Psychol Bull48, 156–158.
65.
WilsonDJ (2019) The harmonic meanp-value for combining dependent tests. Proc Natl Acad Sci U S A116, 1195–1200.
66.
JohnssonP, LipovichL, GranderD, MorrisKV (2014) Evolutionary conservation of long non-coding RNAs; sequence, structure, function. Biochim Biophys Acta1840, 1063–1071.
67.
KwartD, GreggA, ScheckelC, MurphyEA, PaquetD, DuffieldM, FakJ, OlsenO, DarnellRB, Tessier-LavigneM (2019) A large panel of isogenic APP and PSEN1 mutant human iPSC neurons reveals shared endosomal abnormalities mediated by APP beta-CTFs, not Abeta. Neuron104, 1022.
68.
CorsiGI, GadekarVP, HaukedalH, DonchevaNT, AnthonC, AmbardarS, PalakodetiD, HyttelP, FreudeK, SeemannSE, GorodkinJ (2023) The transcriptomic landscape of neurons carrying PSEN1 mutations reveals changes in extracellular matrix components and non-coding gene expression. Neurobiol Dis178, 105980.
69.
DongY, NewmanM, PedersonSM, BarthelsonK, HinN, LardelliM (2021) Transcriptome analyses of 7-day-old zebrafish larvae possessing a familial Alzheimer’s disease-like mutation in psen1 indicate effects on oxidative phosphorylation, ECM and MCM functions, and iron homeostasis. BMC Genomics22, 211.
70.
BarthelsonK, BaerL, DongY, HandM, PujicZ, NewmanM, GoodhillGJ, RichardsRI, PedersonSM, LardelliM (2021) Zebrafish chromosome 14 gene differential expression in the fmr1hu2787 model of fragile X syndrome. Front Genet12, 723.
