Additional file 1 of Integrative single-cell transcriptomic analyses reveal the cellular ontological and functional heterogeneities of primary and metastatic liver tumors

Additional file 1: Figure S1. Overview of the single-cell atlas from primary and metastatic liver tumors and non-tumor tissues. Figure S2. Characteristic heterogeneity of B cells in primary and metastatic liver tumors. Figure S3. Ontological and functional changes of CD4+ T cells in primary and metastatic liver tumors. Figure S4. Functional changes and clinical relevance of CD8+ T cell signatures in primary and metastatic liver tumors. Figure S5. Characteristics of myeloid cells in primary and metastatic liver tumors. Figure S6. Clinical relevance and spatial distribution of macrophage signatures in primary and metastatic liver tumors. Figure S7. Spatial distributions of the fibroblasts, the involved ligands, the malignant epithelial cells and the involved receptors in metastatic liver tumors

Combined effects of the genetic variants in the <i>PTEN</i>, <i>AKT1</i>, <i>MDM2</i> and <i>p53</i> genes on the risk of nasopharyngeal carcinoma.

<p>Abbreviations: OR, odds ratio; CI, confidence interval.</p>a<p><i>χ²</i> test for the distribution of genotypes between patients and control subjects.</p>b<p><i>P</i> values were calculated by multivariate logistic regression, adjusted for age, sex, smoking and drinking status, smoking level, and nationality.</p>c<p><i>χ</i>² test for the <i>P</i>_trend value of genotypes between patients and control subjects.</p>d<p>Low-risk group, individuals carrying 0–2 risk genotypes; high-risk group, individuals carrying 3-4 risk genotypes.</p><p>*<i>P</i> value remained significant after c°rrection for multiple comparisons (<i>P</i> = 0.048).</p

Primers and restriction enzymes used to investigate polymorphisms in the <i>PTEN</i>, <i>AKT1</i> and <i>p53</i> genes.

a<p>Italicized lowercase letters indicate base mismatches.</p>b<p>Designated rs2498799 in previous literature.</p

Haplotypes of <i>AKT1</i> polymorphisms and the risk of nasopharyngeal carcinoma.

<p>(<i>a</i>) Genomic structure of the <i>AKT1</i> locus and the polymorphic sites used. Exons (boxes) and introns are not drawn to scale; open boxes represent noncoding sequences, and filled boxes represent coding sequences. The physical distance between SNPs is shown in nucleotides. (<i>b</i>) Linkage disequilibrium (LD) map of SNPs based on <i>D</i> ´. (<i>c</i>) LD map of SNPs based on <i>r</i>². (<i>d</i>) Global <i>P</i> values from single-locus and multi-locus (two to five) based association analysis. (<i>e</i>) Haplotypes showing significant genetic associations with the risk of nasopharyngeal carcinoma. The two-SNP core haplotype is highlighted in gray.</p

Stratification analysis of the combined genotypes of the <i>PTEN</i>, <i>AKT1</i>, <i>MDM2</i> and <i>p53</i> polymorphisms and risk of nasopharyngeal carcinoma.

<p>Abbreviations: OR, odds ratio; CI, confidence interval.</p>a<p>ORs and <i>P</i> values were calculated by multivariate logistic regression, adjusted for age, sex, smoking and drinking status, smoking level and nationality when appropriate within the strata.</p>b<p>For differences in ORs within each stratum.</p>c<p>Low-risk group, individuals carrying 0–2 risk genotypes; high-risk group, individuals carrying 3–4 risk genotypes.</p

L'Écho : grand quotidien d'information du Centre Ouest

31 août 19181918/08/31 (A47).Appartient à l’ensemble documentaire : PoitouCh