| Literature DB >> 26104294 |
E Nigro1, E Imperlini2,3, O Scudiero1,4, M L Monaco1, R Polito1, G Mazzarella5, S Orrù1,6, A Bianco7, A Daniele8,9.
Abstract
BACKGROUND: Lung cancer is a leading cause of mortality. The most common cancer subtype, non small cell lung cancer (NSCLC), accounts for 85-90% all cases and is mainly caused by environmental and genetic factors. Mechanisms involved in lung carcinogenesis include deregulation of several kinases and molecular pathways affecting cell proliferation, apoptosis and differentiation. Despite advances in lung cancer detection, diagnosis and staging, survival rate still remains poor and novel biomarkers for both diagnosis and therapy need to be identified. In the present study, we have explored the potential of novel specific biomarkers in the diagnosis of NSCLC, and the over-expression/activation of several kinases involved in disease development and progression.Entities:
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Year: 2015 PMID: 26104294 PMCID: PMC4487583 DOI: 10.1186/s12931-015-0234-2
Source DB: PubMed Journal: Respir Res ISSN: 1465-9921
Fig. 1ERK1/2 and AKT kinases are significantly more activated in NSCLC than in control lung tissues. a One representative western blotting image and graphical representation of pixel quantization of p-ERK1/2 and relative total ERK1/2 of 8 lung tissue specimens. b One representative western blotting image and graphical representation of pixel quantization of p-AKT and relative total AKT of 8 lung tissue specimens. Each experiment was performed three times in duplicate.* = p < 0.05 by t-test analysis. For other details see materials and methods
Fig. 2NF − κβ and p-IKBα are significantly more expressed in NSCLC than in control lung tissues. a One representative western blotting image and graphical representation of pixel quantization of NF − κβ and relative total GAPDH of 8 lung tissue specimens. b One representative western blotting image and graphical representation of pixel quantization of p-IKBα and total IKBα in 8 lung tissue specimens. Each experiment was performed three times in duplicate.* = p < 0.05 by t-test analysis. For other details see materials and methods
Fig. 3Differential protein expression profile between pooled tumour and control samples from 8 NSCLS patients (6 with histotype of AC and 2 with histotype of ASC). Arrow indicates protein band associated to CAI and CAII isoforms identification. For other details see materials and methods
Identified proteins in control and NSCLC tissues by MS analysis
| Protein | Gene | Gene ID | MWa | Mascot Scoreb | Mascot Scoreb |
|---|---|---|---|---|---|
| [Peptide]c | [Peptide]c | ||||
| NSCLC | Control | ||||
| lactoferrin precursor | LTF | 12083188 | 80214 | 946 [15] | 298 [5] |
| transferrin | TF | 37747855 | 79310 | 581 [9] | 940 [15] |
| 78 kDa glucose-regulated protein precursor | HSPA5 | 16507237 | 72402 | 507 [8] | 503 [8] |
| moesin | MSN | 4505257 | 67892 | 412 [8] | 396 [7] |
| myeloperoxidase, isoform CRA_d | MPO | 119614879 | 76923 | 331 [6] | 73 [1] |
| protein disulfide-isomerase A4 precursor | PDIA4 | 4758304 | 73229 | 191 [3] | 128 [2] |
| glyceraldehyde-3-phosphate dehydrogenase | GAPDH | 31645 | 36201 | 581 [9] | 375 [6] |
| annexin A2 isoform 2 | ANXA2 | 18645167 | 38808 | 975 [16] | 504 [10] |
| annexin A1 | ANXA1 | 4502101 | 38918 | 587 [8] | 522 [7] |
| L-lactate dehydrogenase A isoform 1 | LDHA | 5031857 | 36950 | 391 [7] | N. D.d |
| aldolase A | ALDOA | 28614 | 39706 | 240 [4] | 65 [1] |
| peroxiredoxin-1 | PRDX1 | 4505591 | 22324 | 158 [3] | 253 [5] |
| Aldo-keto reductase family 1 member C4 | AKR1C4 | 308153631 | 37442 | 155 [3] | N. D.d |
| 60S acidic ribosomal protein P0 | RPLP0 | 4506667 | 34423 | 133 [2] | N. D.d |
| Actin, beta | ACTB | 16359158 | 42078 | 103 [2] | 238 [4] |
| alcohol dehydrogenase beta subunit | ADH1B | 178098 | 40665 | N. D.d | 107 [2] |
| cathepsin D | CTSD | 157879206 | 26511 | 151 [3] | 131 [2] |
| stomatin | STOM | 14715077 | 31958 | 112 [2] | N. D.d |
| apolipoprotein A-I, isoform CRA_b | APOA1 | 177827 | 23454 | 566 [9] | 1057 [17] |
| ribosomal protein L7 | RPL7 | 1335288 | 29907 | 170 [2] | 75 [1] |
| tyrosine 3-monooxygenase/tryptophan 5-monooxygenase activation protein, gamma | YWHAG | 380765197 | 28373 | 169 [2] | 96 [1] |
| tyrosine 3-monooxygenase/tryptophan 5-monooxygenase activation protein, beta polypeptide variant | YWHAB | 62089104 | 22563 | 48 [1] | 113 [2] |
| triosephosphate isomerase 1 | TPI1 | 136066 | 26894 | 633 [10] | 394 [6] |
| proteasome subunit alpha type-6 | PSMA6 | 8394076 | 27838 | 184 [3] | 65 [1] |
| carbonic anhydrase 1 | CA1 | 4502517 | 28909 | 104 [2] | 482 [8] |
| carbonic anhydrase 2 | CA2 | 15080386 | 29215 | N. D.d | 237 [4] |
| azurocidin | AZU1 | 28977 | 27093 | 130 [2] | N. D.d |
| phosphoglycerate mutase 1 | PGAM1 | 4505753 | 28900 | 91 [2] | N. D.d |
| enoyl-CoA hydratase | EHHADH | 1922287 | 31807 | 107 [2] | N. D.d |
| profilin-1 | PFN1 | 4826898 | 15216 | N. D.d | 103 [2] |
| endoplasmic reticulum protein 29, isoform CRA_b | ERP29 | 119618398 | 29638 | 102 [2] | N. D.d |
| pre-serum amyloid P component | APCS | 337758 | 25495 | 337 [5] | 318 [5] |
| peroxiredoxin-6 | PRDX6 | 134254698 | 25011 | 342 [6] | 299 [5] |
| MHC class II antigen | HLA-DRB1 | 10185082 | 30525 | N. D.d | 183 [3] |
| MHC class I antigen | HLA-DQB | 325656872 | 21947 | N. D.d | 150 [3] |
| Rab5c-like protein | RAB5C | 508285 | 23781 | 101 [2] | 97 [2] |
| proteasome subunit beta type-4 | PSMB4 | 22538467 | 29242 | N. D.d | 211 [3] |
| rho GDP-dissociation inhibitor | ARHGDIB | 56676393 | 23031 | N. D.d | 122 [2] |
aTheoretical MW
bProtein score assigned by Mascot software is derived from ion scores that are -10*Log [p], where p is the probability that the observed match is a random event
cNumber of peptides matched
dNot determined
Spectral counting and protein ratios for differentially expressed proteins
| Protein | Gene | NSAFa | NSAFa | Rsc b |
|---|---|---|---|---|
| NSCLC | Control | |||
| carbonic anhydrase 2 | CA2 | 0 | 0,00693 | 3,10 |
| MHC class I antigen | HLA-DQB | 0 | 0,0131 | 2,43 |
| alcohol dehydrogenase beta subunit | ADH1B | 0 | 0,00356 | 2,43 |
| carbonic anhydrase 1 | CA1 | 0,00559 | 0,0180 | 2,10 |
| profilin-1 | PFN1 | 0 | 0,00513 | 1,94 |
| MHC class II antigen | HLA-DRB1 | 0 | 0,00931 | 1,94 |
| rho GDP-dissociation inhibitor | ARHGDIB | 0 | 0,00393 | 1,94 |
| aldolase A | ALDOA | 0,00591 | 0,000974 | -1,61 |
| ribosomal protein L7 | RPL7 | 0,00869 | 0,00143 | -1,61 |
| enoyl-CoA hydratase | EHHADH | 0,00250 | 0 | -1,97 |
| lactoferrin precursor | LTF | 0,0124 | 0,00154 | -2,25 |
| proteasome subunit alpha type-6 | PSMA6 | 0,0174 | 0,00144 | -2,52 |
| Aldo-keto reductase family 1 member C4 | AKR1C4 | 0,00579 | 0 | -2,71 |
| stomatin | STOM | 0,00604 | 0 | -2,71 |
| 60S acidic ribosomal protein P0 | RPLP0 | 0,00807 | 0 | -3,20 |
| phosphoglycerate mutase 1 | PGAM1 | 0,0107 | 0 | -3,20 |
| endoplasmic reticulum protein 29, isoform CRA_b | ERP29 | 0,00894 | 0 | -3,20 |
| myeloperoxidase, isoform CRA_d | MPO | 0,0184 | 0,00076 | -3,48 |
| L-lactate dehydrogenase A isoform 1 | LDHA | 0,00859 | 0 | -3,57 |
| azurocidin | AZU1 | 0,0161 | 0 | -3,86 |
aNormalized Spectral Abundance Factor
bRsc is calculated according to semi-quantitative parameter proposed by Old [42] and represents the log2 ratio between the protein expression level of control vs the protein expression level of NSCLC tissues. Proteins with Rsc ≥ 1,50 or ≤ -1,50 were considered differentially expressed
Fig. 4Western blot analysis confirms CAI and CAII as the two most differentially expressed proteins in NSCLC compared to control tissues. One representative western blot image (a) and graphical representation of pixel quantization (b) of CAI and CAII in lung tissues from 3 NSCLC patients (3 with histotype of AC and 1 with histotype of ASC). Each experiment was performed three times in duplicate* = p < 0.05 by t-test analysis. For other details see materials and methods