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. 2022 May 25;23(11):5914. doi: 10.3390/ijms23115914

Table 1.

Details of the included studies. (NS = non specified).

Study Design (Level of Evidence) Study Population Age
(Mean/Range)
Gender
Ethnicity Spine Deformity Initial Cobb Angles
(Mean/Max)
Follow-Up Period Curve Progression Definition Biologic Sample Technique Gene/s Involved
Polymorphism
Results Authors
Retrospective case series (IV) 304 girls with AIS (main curve < 10°) 12.5 ± 1.6 years
100% female
Japanese 189 double curves
62 right thoracic curve,
25 thoracolumbar curves
13 lumbar curves
15 triple curves
24.6 ± 10.0°

31.3 ± 12.6°
>1 year until growth maturation when height no longer changes progression of 5° from initial evaluation DNA from peripheral blood lymphocytes PCR-RFLPs ER gene

Polymorphic first intron PvuII site and
the XbaI site
XbaJ polymorphism in the ER gene associated with curve progression
(p = 0.03).
M. Inoue (2002)
Retrospective case series (IV) 304 girls with AIS (main curve < 10°) 12.5 ± 1.6 years
100% female
Japanese 189 double curves
62 right thoracic curve,
25 thoracolumbar curves
13 lumbar curves
15 triple curves
24.6 ± 10.0°

31.3 ± 12.6°
>1 year until growth maturation when height no longer changes progression of 5° from initial evaluation DNA from peripheral blood lymphocytes PCR-RFLPs MED4
ESR1
CYP17A1
The XbaJ polymorphism in the ER gene was associated with curve progression
(p = 0.03).
M. Inoue
(2002)
Retrospective case series (IV) 340 AIS female patients 12–16

100% female
Chinese NS ≥20° Until skeletal maturity, 16 years, or surgical intervention NS Peripheral blood sample PCR-RFLD IGF-I

Rs5742612 and rs2288377
Cobb’s angle higher in patients with TT genotype p = 0.04) Y. Yeung
(2006)
Retrospective Case-control study
(III)
540 AIS patients

260 healthy controls

(A subgroup of 364 AIS patients had
been followed up to skeletal maturity at age 16)
AIS patients:
13.4 ± 1.4
Female: 540 (100%)

Healthy controls:
13.3 ± 1.3
Female: 260 (100%)
Chinese -King III (24.9%)
-thoracolumbar (22.6%).
-King I 14.5%
-King II 16.2%
-King V (6.8%)
-lumbar curve (8.3%)
-triple curve (6.6%).
28.9° ± 11.5° Until skeletal maturity at age 16 Curve progression was defined as increase in Cobb
angle with greater than 5° from the initial evaluation.
Peripheral blood sample PCR-RFLD ER gene

Two common SNPs (PvuII and XbaI)
in the intron 1 of ESR1
No association between curve severity and curve progression and the two SNPS (Pvull and XbaI) N. Tang
(2006)
Retrospective Case-Control Study (III) 419 AIS patients

750 healthy controls
AIS patients:
16.1 ± 0.93,
(12–19),
89.8% female

Healthy controls:
15.8 ± 0.10,
(8–24),
88.3% female
Chinese NS High-risk genotype: 32.11° ± 11.67°

Intermediate-risk genotype: 32.25° ± 12.42°

High-risk genotype: 37.91° ± 17.1°
more
than 12 months until the age of growth maturation (16 years
old)
NS Peripheral blood leukocytes PCR-RFLD MATN1 gene (matrilin 1 gene): rs1188402, rs1065755 rs1149045, rs1149046, rs3828051,
rs1149048,
rs12404006
Genotype GG of Rs1149048 SNPs
was
statistically significant with the mean maximal Cobb angle.
Z. Chen
(2009)
Retrospective cohort study (III) 67 AIS patients with double curve

100 healthy controls
AIS patients:
15.09 ± 2.37, 10–20
7.8% male
82.2% female

Healthy controls:
15.55 ± 2.21, 10–19
25% male
75% female
Chinese 40 thoracic curves
12 thoracolumbar curves
15 lumbar curves
The Cobb angle of the major curve of AIS
ranged from 30° to 90°. There were 60 patients with Cobb
angle >40°.
NS Cobb angle >30 Peripheral blood sample PCR ER1
CALM1

ER1 gene:
rs2234693,
allele T;

CALM 1 gene:
rs12885713,
allele T
Significant association between double curve and CALM1 ER1 SNPs, and between Cobb angle and SNPs of ER1 gene (0.0128) D. Zhao
(2009)
Retrospective Cohort study (III) Screening group (277):
-Severe: 8 (3%)
-Moderate: 34 (12%)
-Mild: 235 (85%)

Spine surgery practice group (257):
-Severe: 28 (11%)
-Moderate: 54 (21%)
-Mild: 175 (68%)

Male group (163):
-Severe: 18 (11%)
-Moderate: 18 (11%)
-Mild: 127 (78%)
9–13 at diagnosis

Screening group: Female: 277 (100%)

Spine surgery group: Female: 257 (100%)
Caucasian NS >10° Until skeletal maturity or sever curve -Progression to a severe curve: Cobb angle >40° in an individual still growing.
Cobb angle >50° in an individual not growing
-Progression to a moderate curve: Cobb angle of 25° or greater but not reaching the severe range by skeletal maturity
Saliva samples Quantitative PCR 53 SNPs identified with a previous GWAS

The authors stated a prognostic test algorithm (AIS-PT, Scoliscore) with a scale (1–200) based on 53
SNP markers, cut point 40: 1–40 (≤1% risk of progression)
Low-risk scores (<41) had NPV of 100%, 99%, and 97%, respectively, in the tested
populations. (95% CI: 98.6–100.0).
K. Ward
(2010)
Retrospective case series (IV) 312 AIS patients:

-90 failures of the brace treatment
-222 successes of the brace treatment
12.7 ± 1.5, (10–15)

Female: 41 (87%)
Male: 41 (13%)
Chinese Single thoracic curve 128 (32.1%)

Single thoracolumbar
or lumbar curve
66 (30.3%)

Double major curve 118 (24.5%)
<30: 195 patients

≥30: 117
14.4 ± 4.8 months, (7.2 ± 26.4) Curve progression of more than 5° compared to the initial Cobb angle

Surgical intervention because of curve progression.
Peripheral blood sample PCR-FLP Single nucleotide polymorphism (SNP) sites in the genes for
estrogen receptor a (rs9340799), estrogen receptor b (rs1256120),
tryptophan hydroxylase 1 (rs10488682)
melatonin receptor 1B
(rs4753426), and matrillin-1 (rs1149048),
Statistically significant differences between the two groups in SNP rs9340799 in ERa. L. Xu
(2011)
Retrospective Case-control study (III) 362 AIS patients
377 age-matched controls

120 skeletally immature AIS patients who received continuous brace treatment for minimum of 2 years
AIS patients:
15.30 ± 2.49
10–20
91.9% female

Controls:
15.86 ± 0.93
14–18
90.2% female
Chinese Thoracic and thoracolumbar curves 25°–40° 30 ± 4.2 months Curve progression of more than 5° compared to the initial Cobb angle Peripheral blood sample PCR-RFLP NTF3 gene:
rs1805149 SNP rs11063714 SNP
rs11063714 SNP significantly associated with lower mean maximum Cobb angle and brace treatment success Y. Qiu
(2012)
Retrospective case-control study (III) 529 AIS case

512 healthy controls
AIS case:
14.54 ± 1.62 (1–18)
Female: 529 (100%)

Healthy controls:
14.36 ± 1.93 (11–18)
Female: 512 (100%)
Chinese Thoracic curve AIS case:
Mean Maximum Cobb: 38.30° ± 16.71°, (20°–100°)
NS NS Peripheral blood sample PCR-RFLP IL-17RC gene

Rs708567
GG genotype of Rs708567 showed significant association with higher Cobb angle S. Zhou
(2012)
Retrospective Case-Control study (III) 53 cases of AIS

54 controls
AIS group:
14.9 ± 3.4
9–19

Females: 46 (86.8%)
Males: 7 (13.2%)

Control group:
29.8 ± 5.5
18–40
Females: 51 (94.4%)
Males: 3 (5.6%)
Turkish NS 29.88° ± 11.78° NS NS Peripheral blood samples RT-PCR MCM6:
6p21; 13910; 4988235

MATN1:
1p35; 1149048

VDR BsmI:
12q13.1; 1544410
There was no statistical difference (p < 0.05) between case and control in terms of progression of the curve H. Yilmaz
(2012)
Retrospective case-control study (III) 300 AIS patients

300 Healthy controls
AIS group:
-12.8 ± 2.1
Female 156 (52%)
Male: 144 (48%)

Controls:
13.3 ± 2.8
Female: 160 (53.3%)
Male: 140 (46.7%)
Russian Thoracic: 167 (56.1%)
Thoraco-lumbar: 117 (39.2%)
Lumbar: 14 (4.7%)
10°–19°: 154 (51.3%)
20°–29°: 116 (38.7%)
30–39°: 20 (6.7%)
<39°: 10 (3.3%)
36 months NS Peripheral blood sample RT-PCR TGF!
Rs1800469
Rs1800471
TGFB1 gene is associated with curve severity and progression in AIS. I. Ryzhkov (2013)
Retrospective Case-control study (III) 949 AIS patients


976 age-matched normal control subjects
AIS group:
820 girls and 129 boys

Control group: 662 females and 314
males
Chinese NS >20° NS NS Peripheral blood sample PCR-RFLP LBX1 (ladybird homeobox 1) gene on chromosome 10q24.31.

SNP rs11190870 near LBX1
TT genotype of rs11190870
Significantly associated with larger Cobb angle
H. Jiang
(2013)
Retrospective Case-Control study (III) 68 AIS patients:
-33 lower-risk group: Cobb’s angle 10–40
-35 high-risk group: Cobb’s angle >40°

35 age-/sex-matched controls
AIS group:

-low-risk: 14.5
26 (80.6%) females
7 (19.4%) males

-high risk:
14.9
9 (25%) males
26 (75%)
females

Control group:
13.4
9 (25%) males
26 (75%)
females
Korean NS Low risk: 25.8°

High risk: 58.8°
NS NS Peripheral blood samples PCR-RFLP CHL1 (rs10510181)
DSCAM (rs2222973)
LAPTM4B (rs2449539)
FOXB1 (rs1437480)
CBLN4 (rs448013)
RRAGC (rs10493083)
BRIP1 (rs16945692)
MATN1 (rs1149048)
MTNR1B (rs4753426)
IGF1 (rs5742612)
LAPTM4B rs2449539 significantly associated with higher risk of progression. E. Moon
(2013)
Retrospective Comparative study
(II)
2217 AIS patient
-progression group (880 patients)

-non-progression group (492)
Progression group: 17.2
Female: 830 (94.3%)
Male: 50 (5.7%)
Non-progression group: 16.8
Female: 469 (95.3%)
Male: 23 (4.7%)
Japanese Thoracic curve: 819 (93%)

Non-Thoracic curve: 61 (7%)
>10° NS >40°
progression group

<30° and skeletal maturation
Non-progression group
Peripheral blood sample PCR neurotrophin 3
(rs1063714)
G protein-coupled estrogen receptor
(rs3808351, rs10269151
rs4266553)
tissue inhibitor of metalloproteinase
(rs8179090)
No statistical difference was found
between the 4 SNPs and AIS curve progression
Y. Ogura
(2013)
Retrospective cohort study (III) 405 European AIS patients:
-rare variants: 26
-No rare variants: 379

370 Chinese Han AIS patients:
-rare variants: 28
-No rare variants: 342

47 Other ancestries AIS patients
European AIS
-No rare variants:
Female: 326 (86%)
Male: 53
-Rare variants:
Female: 22 (83%)
Male: 3 (17%)
European and Chinese Right thoracic and thoracolumbar curves >10° NS NS Peripheral blood sample Exome sequencing Rare damaging variants of FNB1 and FNB2 FBN1 or FBN2 variant was associated with curve magnitude J. Buchan
(2014)
Retrospective Case-control study (III) 248 AIS patients:
-Non-progressive IS: 90
-Slowly progressive IS: 90
-rapidly progressive IS (RP-IS): 62

243 healthy female controls
NS Polish Thoracic curve: 191 (77%)
Lumbar curve: 51 (20.5%)
Single curve: 97 (39%)
Double curve: 145 (58.5%)
NS 3 years The change of Cobb angle value on 2 consecutive radiographs taken at 6 months of distance Peripheral blood samples PCR-RFLP ESR2 gene:
Promoters:
Alw NI
(rs1256120)
AluI
(rs4986938)
Rsa I
(rs1256049)
There was a difference
of genotype distribution of rs4986938 between progression and non-progression groups.
T. Kotwicki
(2014)
Retrospective cohort study (II) 126 AIS patients
-Progression group: 27 (21%) patients
-Non-progression group: 99 (79%)
12.2 ± 1.2
(9–15.8)
113 female (89.7%)
31 males
(10.3%)
Caucasian NS 10°–25° 28.5 ± 9.9 months Patients who had curve progression
to >40 or had undergone a spinal fusion
Saliva sample Quantitative PCR Prognostic test algorithm (AIS-PT, Scoliscore) with a scale (1–200). Cut point: Low risk (1 to 50 points), intermediate risk (51 to 179 points), or high risk (180 to 200 points). No significant association between the continuous
ScoliScore value and curve progression
(p = 0.720).
B. Roye
(2015)
Retrospective cohort study (III) 148 patients with severe AIS:
-302 patients with non-severe AIS
-901 healthy controls
Severe AIS:
15 ± 2 years
(10–25)
Females: 129 (87.2%)
Males: 19 (12.8%)

Non-severe AIS
16 ± 1 years
(14–22)
Females: 259 (85.7%)
Males: 43 (14.3%)
French-Canadian NS 56° ± 12°
(37°–90°)
NS NS Peripheral blood sample Quantitative PCR The authors stated a prognostic test algorithm (AIS-PT, Scoliscore) with a scale (1–200) based on 53
SNP markers.
None of the SNPs used were associated. Q. Tang
(2015)
Retrospective case series (IV) 16 AIS patients 12.5
(10–15)
Caucasian NS 25.2°
(20°–33°)
2.3 years

(1–4
At least 1 year after brace treatment or skeletal maturity)
Cobb >45° Saliva sample Quantitative PCR Prognostic test algorithm (AIS-PT, Scoliscore) with a scale (1–200). Cut point:160; 160–200 (high risk of curve progression with Cobb >45°) vs. <160 (low risk of curve progression with Cobb >45°) The mean
ScoliScore among those who progressed to more than 45 degrees was higher than that
among those who did not (176 vs. 112, p = 0.030).
D. Bohl
(2016)
Case-only study (IV) 670 AIS patients
-313 in non-progression group
-357 in progression group
-Non-progression group:
12.3 ± 2.5
-Progression group:
12.5 ± 2.7 years
Chinese NS -22.6° ± 3.7° for non-progression group
-53.4° ± 12.7° for progression group.
NS -Cobb angle <25° at final follow-up: non-progression
group.
-Cobb angle >40°: progression group.
Peripheral blood sample Quantitative PCR The authors stated a prognostic test algorithm (AIS-PT; Scoliscore) with a scale ranging from 1 to 200 Allele A of rs9945359 was significantly higher in the
progression group than in the non-progression group (p = 0.01).
L. Xu
(2016)
Genome-wide association study (GWAS)
(II)
2142 patients with AIS

1105 in progression group

832 in non-progression group

205 patients excluded
NS Japanese NS NS NS Progression group: Cobb angle 40°

Non-progression: Cobb
Angle 30° in skeletally mature patients
Peripheral blood sample NS MIR4300 microRNA host gene

(SNP rs1828853)
rs1828853 showed association with progression of AIS. Y. Ogura
(2017)
Retrospective Case-control study (III) 2645 AIS patients

2746 healthy controls

(And further replicated in 693 patients and 254 controls.)
12.5 ± 2.1 years for the patients

16.9 ± 2.8 years for the controls
Chinese NS 56.2 ± 14.3° NS NS Peripheral blood sample and bilateral intraoperative facet joint tissue SNP Genotyping Assay BNC2
(rs10738445)
Genotype CC h larger
Cobb angle
L. Xu
(2017)
Case only study (IV) 1860 Patients with AIS
-594 mild curve
-326 moderate curve
-940 severe curve
10–18 years

Females: 1763 (94.7%)
Males: 97 (5.3%)
Japanese NS Severe curve: 54.8° ± 12.1°

Mild curve: 24.4° ± 4.0°
NS -Severe curve: Cobb angle of 40)
-mild curve: Cobb angle <30.
Peripheral blood sample PCR-RFLP LBX1 (ladybird homebox 1) 10q24.31

SNP rs11190870
No significant
differences were observed between the groups
Y. Takashi
(2018)
Retrospective case-control study (III) 319 AIS patients

201 age-matched female healthy controls
AIS patients:
14.3 ± 2.2; 10–16

Controls:
13.7 ± 1.2; 10–16
Chinese major right thoracic curvature
and major non-thoracic curvatures
Cobb >10° Until skeletal maturity or surgery -Progressive curve group: Cobb >40°
-non-progressive curve group: Cobb angle <40
Peripheral blood samples PCR-RFLP LBX1, BNC2, SOX9/KCNJ2, GPR126, AJAP4, BCL-2, PAX3/ EPHA4, LBX1 (LBX1-
AS1).

SNPs:
rs11190870, rs12946942, rs13398147, rs241215,
rs3904778, rs6570507, and rs678741
There was no association found between the seven SNPs with curve progression in AIS G. Man
(2018)
Prospective Case-control study (III) 92 AIS patients:
-50 patients in the progression group
-42 patients in the non-progression group

276 unrelated subjects:
-112 in progression group
-164 in non-progression group
AIS patients:
-Progression group: 13.7 ± 2.4
Female: 37 (74%); Male: 13 (26%)

-Non progression group: 13.3 ± 1.9
Female: 30 (71%);
Male: 12 (29%)

Unrelated subjects:
-Progression group: 14.1 ± 2.1
Female: 85 (76%);
Male: 27 (24%)

-Non progression group: 13.8 ± 2.7
Female: 126 (76.8%)
Male: 38 (23.2%)
Chinese Single thoracic,
thoracolumbar, single lumbar, double thoracic, and double lumbar
AIS patients:
-Progression group curve > 45° 
-Non-progression group curve <30°

Unrelated subjects:
10° < curve > 25°
Until skeletal maturity curve progression
of at least 5° in two successive clinical follow-ups
Peripheral blood sample Oligonucleotide Ligation and
Detection system
The genome and methylome of peripheral monocytes were sequential Methylation levels of site Cg01374129 (Has2 gene)
were significantly lower in the progression group than in the non-progression group.
Y. Meng
(2018)
Retrospective case-control study (III) AIS patients: 13

Non-AIS controls: 10
AIS patients: 15.54 ± 1.76


Non-AIS patients: 15.60 ± 5.77
Chinese NS AIS patients:
58.15° ± 11.41°
NS NS Human bone-derived primary bone cells from iliac crest bone tissue and serum RT quantitative PCR MiR-145 of Wnt/ß catenin Significant
negative correlations between circulating miR-145 and serum sclerostin, osteopontin, and osteoprotegerin.
J. Zhang
(2018)
Retrospective case-control study (III) 50 patients with AIS

50 healthy controls
AIS patient:
12.98 ± 1.46
Female: 46 (92%)
Male: 4 (8%)

Healthy controls:
12.46 ± 1.59
Female: 45 (90%)
Male: 5 (10%)
Chinese NS 29 AIS patients > 40°

21 AIS patients < 40°
NS NS Peripheral blood sample PCR and pyrosequencing COMP gene promoter methylation AIS patients with different levels of methylation showed significant differences in
Cobb angle of main curve
(p = 0.011)
S. Mao
(2018)
Retrospective Case-control study (III) I960 AIS patients

1499 healthy subjects
AIS group:
14.3 ± 3.2

Healthy group:
22.5 ± 5.9
Chinese All AIS patients had main thoracic curve AIS patients: 38.58 ± 12.38 NS NS Peripheral blood samples

Intraoperative muscular tissue
RT-PCR FBN 1 & FBN 2

106 SNPs of FBN 1 & FBN2
The expression level of
FBN1 was remarkably correlated with the curve severity
(p.0.02).
F. Sheng
(2018)
Retrospective Case-control study (III) 50 patients with AIS

50 healthy controls
AIS patients:
22 patients: 10–13
28 patients: 14–16
Female: 46 (92%)
Male: 4 (8%)
Chinese Thoracic or thoraco-lumbar curve Cobb from 10° to 50° NS NS Peripheral blood sample Pyrosequencing PITX1

PITX1 promoter methylation
The methylation level of 6 CpG sites in PITX1 promoters was significantly associated with Cobb angle. B. Shi
(2018)
Retrospective Case-control study (III) 5 AIS patients:
-10 paraspinal muscle samples

60 Validation non-AIS patients
AIS patients:
-14.2 ± 1.92 years
-5 female (100%)

Validation non-AIS patients:
-15.25 ± 2.64
-49 female (81.6%)
-11 male (19.4%)
Chinese AIS patients:
-Lenke 1: 3
-Lenke 3: 1
-Lenke 4: 1

Validation non- AIS patients:
-Lenke 1: 34
-Lenke 2: 3
-Lenke 3: 15
-Lenke 4: 8
AIS patients:
56.8° ± 6.06°

Validation non- AIS patients:
54.48° ± 10.09°
NS NS Intraoperative paraspinal muscular samples RNA sequences + Quantitative RT-PCR ADIPOQ mRNA and H19 mRNA ADIPOQ mRNA and H19mRNA showed statistical significance (p < 0.001 and p = 0.04, respectively) H. Jiang
(2018)
Retrospective Case-control study (III) 100 AIS patients:
-53 progressive curves
-47 non-progressive curves

100 healthy controls
AIS patients:
12.7 ± 1.5
Female: 100 (100%)

Healthy controls:
Female: 100 (100%)
Polish Right-sided thoracic curve of Cobb angle greater than 20° (Lenke types 1 and 3). AIS patients:
-Whole group: 31.3°
-Progression group: 35.4
-Non-progression group: 27.7
34.8 ± 21.6 More than 12° of Cobb angle every year Peripheral blood sample PCR-FRET TIMP2

Nine different TIMP2 polymorphism
Four of the polymorphisms showed non-equal distributions in patients with different progression rates. M. Andrusiewicz
(2019)
Retrospective Case-control study (III) 223 AIS patients

375 age-matched controls
AIS patients:
127 patients < 12
96 patients > 12
Female:199 (89%)
Male: 24 (11%)
Chinese Lenke 1: 23
Lenke 2: 110
Lenke 3: 28
Lenke 4: 27
Lenke 5: 29
Lenke 6: 6
130 patients < 23°
93 patients > 23°
11.9 (1.4 months to 31 months) a curve greater than 30° after
skeletal maturity was used to define curve progression
Peripheral blood sample Exome sequencing The authors searched for rare damaging variants (defined as missense, nonsense, frameshift,
or splice-site
variants and variants with a minor allele frequency of <1% in public databases)
The number of rare damaging
variants associated with curve progression
(p < 0.05, OR = 4.304, 95%, CI 2.4 to 7.5
H. Jiang
(2019)
Retrospective Cohort study
(II)
2272 patients with severe AIS

13,859 healthy controls
NS Japanese; Chinese and Scandinavian NS NS NS NS Peripheral blood or saliva sample PCR based 17q24.3 near the genes SOX9 and KCNJ2)

rs12946942
rs12946942 SNP showed significant association in severe AIS patients: K. Takeda
(2019)
Retrospective Case-Control study (III) 50 AIS patients

50 Healthy controls
AIS patients:
-12.6 ± 1.5 years (10–18 years)

Healthy controls:
-12.5 ± 1.6 years (10–18 years)

100 females (100%)
Chinese NS AIS patients:
-20.1° ± 8.3° (10°–60°)
12 months NS Peripheral blood samples RT-PCR PCDH10 gene methylation and expression PCDH10 methylation level significantly correlated to curve severity B. Shi (2019)
Retrospective Case-control study (III) (1) mi-RNA sequencing cohort:

10 AIS patients:
-5 severe curves
-5 mild curves

5 Healthy controls

(2) qPCRT validation cohort:

-40 severe curve
-40 mild curve
-40 healthy controls

(3) Facet joints and bone tissues group:
-21 severe AIS patients
-20 non-scoliosis patients
Mi RNA sequence cohort:
-Severe AIS:
13.0 ± 2.5 years
5 female (100%)
-Mild AIS:
14.2 ± 0.8 years
5 female (100%)
-5 controls:
11.6 ± 2.9 years
5 female (100%)

qPCR cohort:
-Severe AIS:
12.6 ± 2.2 years
27 females (67.5%)
13 males (32.5%)
-Mild AIS:
12.4 ± 1.8 years
30 female (75%)
10 males (25%)
-Healthy controls:
12.2 ± 1.9
28 female (70%)
12 male (30%)
Chinese NS Mi RNA sequence cohort:
-Severe AIS:
64.6° ± 16.7°
-Mild AIS:
26.0° ± 5.8°

qPCR cohort:
-Severe AIS:
61.3° ± 9.5°
-Mild AIS:
22.7° ± 6.7°
NS NS Peripheral blood sample and bone tissue RT-PCR miR-151a-3p and GREM1 expression miR-151a-3p and GREM1 expression significantly correlated to severe AIS curves Y. Wang (2020)
Retrospective case series (IV) 211 AIS patients:
-Non-progressive curve = 80
-Slowly progressive curve = 78
-Rapidly progressive curve = 53

83 healthy subjects
AIS patients:
-Non-progressive: 18.5 ± 1.8 (15.0–24.1)
-Slowly progressive:
16.9 ± 2.4 (15–26.2)
-Rapidly progressive:16.3 ± 7.1 (12.4–50.1)

Female: 211 (100%)
Caucasian NS AIS patients:
-Non-progressive: 23.9 ± 5.4 (10–30)
-Slowly progressive: 38.9 ± 7.9 (30–65)
-Rapidly progressive: 62.7 ± 15.7 (39–114)
12 months The change of
Cobb angle value on the two consecutive X-rays taken at 12-month time intervals expressed in degrees
per month.
Peripheral blood sample PCR-RFLP for:
rs1017861, rs1324842, rs4738813

Sanger sequencing for: rs78874766
rs4738824, rs7479761
CHD7

rs1017861, rs13248429, rs4738813
rs78874766,
rs4738824, and rs74797613.
rs1017861 and
rs4738813 were associated with curve severity and progression rate (p < 0.05).
K. Borysiak
(2020)
Retrospective case-control study (III) 1952 AIS patients:
-747 progression group
-520 non-progression group

2495 healthy controls
AIS group:
-Progression group: 13.2 ± 2.4
-Non progression group: 13.0 ± 2.3

Female: 1952 (100%)
Chinese -1218 (62.4%) main thoracic curve
-476 (24.3%) double major curve
-258 (13.3%) major lumbar curves
36.8 ± 3.2, (22–66) NS Progression group:
-Cobb angle >50° and Risser grade < 3

Non-progression group:
-Cobb angle < 30° and Risser grade >3 at final follow-up
Peripheral blood sample

76 intraoperative muscular tissue
RT-PCR MIR4300 HG gene

rs35333564
Significant difference
between two groups regarding both genotype frequency
and minor allele frequency of rs35333564 in MIR4300 gene.
Y. Wang
(2021)
Retrospective case series (IV) 8 female monozygotic twin pairs (n = 16 patients):
-6 discordant twin pairs (difference in primary curve Cobb angle > 10°)

-2 concordant twin pairs (difference in primary curve < 2°)
All individuals:
-37.3 ± 22.5 years

Female: 16 (100%)
Caucasian NS 39.6° ± 15.3° NS NS Peripheral blood sample Microarray analysis Genome-wide methylation in blood (Differentially methylation region (DMR) promoter enrichment analyses) SNPs hypomethylation associated with curve severity P. Carry
(2021)
Retrospective case series (IV) 29 AIS surgery patients:
-10 patients with Cobb ≤70°
-19 patients with Cobb >70°
All individuals:
14.5 ± 1.5 years (12.1–17.9)
29 female (100%)
Caucasian Main thoracic curve All individuals:
77.4° ± 16.1° (52°–115°)
2 years NS Intraoperative deep paraspinal muscles sample and trapezius muscles PRC and Pyrosequencing Methylation levels of ESR1 regulatory regions DRM1/2 methylation status was significantly associated with curve severity P. Janusz (2021)