Methylation of the PTEN Promoter Leads to PTEN Inactivation in Multiple Myeloma
Aberrant methylation of CpG island of the promoter regions of genes is an important epigenetic mechanism, alternative to deletions or mutations, that cause the silencing of genes involved in carcinogenesis. We therefore investigated epigenetic events involved in multiple myeloma by screening 6 genes...
Saved in:
| Published in: | Blood Vol. 112; no. 11; p. 2717 |
|---|---|
| Main Authors: | , , , , , , , , , , , |
| Format: | Journal Article |
| Language: | English |
| Published: |
Elsevier Inc
16-11-2008
|
| Online Access: | Get full text |
| Tags: |
Add Tag
No Tags, Be the first to tag this record!
|
| Abstract | Aberrant methylation of CpG island of the promoter regions of genes is an important epigenetic mechanism, alternative to deletions or mutations, that cause the silencing of genes involved in carcinogenesis. We therefore investigated epigenetic events involved in multiple myeloma by screening 6 genes of interest for evidence of promoter hypermethylation.
PATIENTS AND METHODS: The methylation patterns of the tumor suppressor genes p16INK4a(p16), E-cadherin (ECAD), FHIT and PTEN (negative regulator of AKT/PKB signalling pathway), Wnt signalling pathway antagonist genes WIF-1 and DKK-3 were determined in the bone marrow aspirates of 50 patients with Multiple Myeloma (MM) (37 at diagnosis; male 22; female 28; 68.8 median age. ISS stage: 47% stage I, 8% stage II and 45% stage III.), using the methylation-specific polymerase chain reaction after DNA bisulphite modification. Ten patients with monoclonal gammopathy of undetermined significance (MGUS) and 4 peripheral blood from controls were also evaluated. For statistical analysis Student t and Chi squared or Fisher exact tests were used.
RESULTS: We found at least one hypermethylated gene in all MM patients. Gene methylation frequencies varied from 6% to 74%. ECAD, FHIT and p16 genes demonstrated a relatively high frequency of aberrant methylation with frequencies of 74%, 69% and 42%, respectively. WIF-1, PTEN, DKK-3 genes showed a low frequency of methylation with values of 28%, 14%, 6%, respectively. The methylation frequencies detected in MGUS were 91.6% for ECAD and FHIT, 41.6% for WIF-1, 16,6% for p16 and DKK3. The difference in methylation profile between MM and MGUS was statistically significant (X2= 37, df=5; p=0.0000). PTEN was found hypermethylated in 7/50 (14%) MM but none of MGUS or control samples were methylated. Of these 6 patients had IgG K isotype, 4 had abnormal cariotype with 13q deletion, one hyperdiploidia, one IgH rearrangements. Two patients were simultaneously hypermethylated in p16 gene promoter. No statistically significant correlation between methylation data and clinical parameters: gender, age, isotype of M component, type of light chain, haemoglobin, serum albumin level, calcium, β2 microglobulin, serum creatinine level, LDH, lytic bone lesions were found for any of examined genes. When correlation with Durie-Salmon Stage disease was tested hypermethylation of p16 and WIF-1 resulted more frequently associated with stage IIIA/B (p values 0.006 and 0.000, respectively). When gene methylation status and cytogenetics abnormalities were compared, we found that aberrant methylation of p16 and ECAD were significantly more frequent in MM patients with chromosome 13 abnormalities as sole entity or with 13q deletion associated to IgH translocations. By contrast, promoter hypermethylation of Wnt signalling antagonist genes was associated with 13q deletion co-occurring with a hyperdiploide cariotype. (X2=17; df=8 p value: 0.000). According to the number of methylated genes observed in each sample 48% MM had 3–4 hypermethylated genes. When differences between methylator phenotype and cytogenetics abnormalities were analyzed we found that 3–4 hypermethylated genes have the tendency to be associated with chromosome 13 abnormalities more often than with hyperdiploide cariotype (p value 0.05).
CONCLUSION: Our results indicate that the accumulation of epigenetic events affecting genes regulating cell cycle control, cell adhesion and apoptosis is a common phenomenon in plasma cell disorders and may further contribute to the phenotype of MM cells. This is the first demonstration of PTEN inactivation as a result of promoter hypermethylation in MM patients. Since talidomide seems to have a role in the PTEN/PI3K/AKT pathway, the PTEN function is worthy to be further investigated in Multiple Myeloma. |
|---|---|
| AbstractList | Abstract
Aberrant methylation of CpG island of the promoter regions of genes is an important epigenetic mechanism, alternative to deletions or mutations, that cause the silencing of genes involved in carcinogenesis. We therefore investigated epigenetic events involved in multiple myeloma by screening 6 genes of interest for evidence of promoter hypermethylation.
PATIENTS AND METHODS: The methylation patterns of the tumor suppressor genes p16INK4a (p16), E-cadherin (ECAD), FHIT and PTEN (negative regulator of AKT/PKB signalling pathway), Wnt signalling pathway antagonist genes WIF-1 and DKK-3 were determined in the bone marrow aspirates of 50 patients with Multiple Myeloma (MM) (37 at diagnosis; male 22; female 28; 68.8 median age. ISS stage: 47% stage I, 8% stage II and 45% stage III.), using the methylation-specific polymerase chain reaction after DNA bisulphite modification. Ten patients with monoclonal gammopathy of undetermined significance (MGUS) and 4 peripheral blood from controls were also evaluated. For statistical analysis Student t and Chi squared or Fisher exact tests were used.
RESULTS: We found at least one hypermethylated gene in all MM patients. Gene methylation frequencies varied from 6% to 74%. ECAD, FHIT and p16 genes demonstrated a relatively high frequency of aberrant methylation with frequencies of 74%, 69% and 42%, respectively. WIF-1, PTEN, DKK-3 genes showed a low frequency of methylation with values of 28%, 14%, 6%, respectively. The methylation frequencies detected in MGUS were 91.6% for ECAD and FHIT, 41.6% for WIF-1, 16,6% for p16 and DKK3. The difference in methylation profile between MM and MGUS was statistically significant (X2= 37, df=5; p=0.0000). PTEN was found hypermethylated in 7/50 (14%) MM but none of MGUS or control samples were methylated. Of these 6 patients had IgG K isotype, 4 had abnormal cariotype with 13q deletion, one hyperdiploidia, one IgH rearrangements. Two patients were simultaneously hypermethylated in p16 gene promoter. No statistically significant correlation between methylation data and clinical parameters: gender, age, isotype of M component, type of light chain, haemoglobin, serum albumin level, calcium, β2 microglobulin, serum creatinine level, LDH, lytic bone lesions were found for any of examined genes. When correlation with Durie-Salmon Stage disease was tested hypermethylation of p16 and WIF-1 resulted more frequently associated with stage IIIA/B (p values 0.006 and 0.000, respectively). When gene methylation status and cytogenetics abnormalities were compared, we found that aberrant methylation of p16 and ECAD were significantly more frequent in MM patients with chromosome 13 abnormalities as sole entity or with 13q deletion associated to IgH translocations. By contrast, promoter hypermethylation of Wnt signalling antagonist genes was associated with 13q deletion co-occurring with a hyperdiploide cariotype. (X2=17; df=8 p value: 0.000). According to the number of methylated genes observed in each sample 48% MM had 3–4 hypermethylated genes. When differences between methylator phenotype and cytogenetics abnormalities were analyzed we found that 3–4 hypermethylated genes have the tendency to be associated with chromosome 13 abnormalities more often than with hyperdiploide cariotype (p value 0.05).
CONCLUSION: Our results indicate that the accumulation of epigenetic events affecting genes regulating cell cycle control, cell adhesion and apoptosis is a common phenomenon in plasma cell disorders and may further contribute to the phenotype of MM cells. This is the first demonstration of PTEN inactivation as a result of promoter hypermethylation in MM patients. Since talidomide seems to have a role in the PTEN/PI3K/AKT pathway, the PTEN function is worthy to be further investigated in Multiple Myeloma. Aberrant methylation of CpG island of the promoter regions of genes is an important epigenetic mechanism, alternative to deletions or mutations, that cause the silencing of genes involved in carcinogenesis. We therefore investigated epigenetic events involved in multiple myeloma by screening 6 genes of interest for evidence of promoter hypermethylation. PATIENTS AND METHODS: The methylation patterns of the tumor suppressor genes p16INK4a(p16), E-cadherin (ECAD), FHIT and PTEN (negative regulator of AKT/PKB signalling pathway), Wnt signalling pathway antagonist genes WIF-1 and DKK-3 were determined in the bone marrow aspirates of 50 patients with Multiple Myeloma (MM) (37 at diagnosis; male 22; female 28; 68.8 median age. ISS stage: 47% stage I, 8% stage II and 45% stage III.), using the methylation-specific polymerase chain reaction after DNA bisulphite modification. Ten patients with monoclonal gammopathy of undetermined significance (MGUS) and 4 peripheral blood from controls were also evaluated. For statistical analysis Student t and Chi squared or Fisher exact tests were used. RESULTS: We found at least one hypermethylated gene in all MM patients. Gene methylation frequencies varied from 6% to 74%. ECAD, FHIT and p16 genes demonstrated a relatively high frequency of aberrant methylation with frequencies of 74%, 69% and 42%, respectively. WIF-1, PTEN, DKK-3 genes showed a low frequency of methylation with values of 28%, 14%, 6%, respectively. The methylation frequencies detected in MGUS were 91.6% for ECAD and FHIT, 41.6% for WIF-1, 16,6% for p16 and DKK3. The difference in methylation profile between MM and MGUS was statistically significant (X2= 37, df=5; p=0.0000). PTEN was found hypermethylated in 7/50 (14%) MM but none of MGUS or control samples were methylated. Of these 6 patients had IgG K isotype, 4 had abnormal cariotype with 13q deletion, one hyperdiploidia, one IgH rearrangements. Two patients were simultaneously hypermethylated in p16 gene promoter. No statistically significant correlation between methylation data and clinical parameters: gender, age, isotype of M component, type of light chain, haemoglobin, serum albumin level, calcium, β2 microglobulin, serum creatinine level, LDH, lytic bone lesions were found for any of examined genes. When correlation with Durie-Salmon Stage disease was tested hypermethylation of p16 and WIF-1 resulted more frequently associated with stage IIIA/B (p values 0.006 and 0.000, respectively). When gene methylation status and cytogenetics abnormalities were compared, we found that aberrant methylation of p16 and ECAD were significantly more frequent in MM patients with chromosome 13 abnormalities as sole entity or with 13q deletion associated to IgH translocations. By contrast, promoter hypermethylation of Wnt signalling antagonist genes was associated with 13q deletion co-occurring with a hyperdiploide cariotype. (X2=17; df=8 p value: 0.000). According to the number of methylated genes observed in each sample 48% MM had 3–4 hypermethylated genes. When differences between methylator phenotype and cytogenetics abnormalities were analyzed we found that 3–4 hypermethylated genes have the tendency to be associated with chromosome 13 abnormalities more often than with hyperdiploide cariotype (p value 0.05). CONCLUSION: Our results indicate that the accumulation of epigenetic events affecting genes regulating cell cycle control, cell adhesion and apoptosis is a common phenomenon in plasma cell disorders and may further contribute to the phenotype of MM cells. This is the first demonstration of PTEN inactivation as a result of promoter hypermethylation in MM patients. Since talidomide seems to have a role in the PTEN/PI3K/AKT pathway, the PTEN function is worthy to be further investigated in Multiple Myeloma. |
| Author | Palmas, Angelo D Monne, Maria Murineddu, Marco Mariane, Erika Fancello, Maria Antonietta Calvisi, Anna Noli, Annalisa Asproni, Rosanna Uras, Antonella Piras, Giovanna Pala, Giuseppina Gabbas, Attilio |
| Author_xml | – sequence: 1 givenname: Giovanna surname: Piras fullname: Piras, Giovanna – sequence: 2 givenname: Giuseppina surname: Pala fullname: Pala, Giuseppina – sequence: 3 givenname: Antonella surname: Uras fullname: Uras, Antonella – sequence: 4 givenname: Anna surname: Calvisi fullname: Calvisi, Anna – sequence: 5 givenname: Maria surname: Monne fullname: Monne, Maria – sequence: 6 givenname: Angelo D surname: Palmas fullname: Palmas, Angelo D – sequence: 7 givenname: Annalisa surname: Noli fullname: Noli, Annalisa – sequence: 8 givenname: Marco surname: Murineddu fullname: Murineddu, Marco – sequence: 9 givenname: Erika surname: Mariane fullname: Mariane, Erika – sequence: 10 givenname: Rosanna surname: Asproni fullname: Asproni, Rosanna – sequence: 11 givenname: Maria Antonietta surname: Fancello fullname: Fancello, Maria Antonietta – sequence: 12 givenname: Attilio surname: Gabbas fullname: Gabbas, Attilio |
| BookMark | eNqFkMFuwjAQRK2KSgXab6h_INTrOHFyRIi2SFA40F4tx94IVyFGjovE3zeQ3nuZ1a52RqM3IaPWt0jIM7AZQMFfqsZ7O_sC4P0-4xLkTe7IGDJeJIxxNiJjxlieiFLCA5l03TdjIFKejcl2g_FwaXR0vqW-pvGAdLdfftBd8EcfMdA1atvR6IfzqtUmuvPw71q6-WmiOzVINxds_FE_kvtaNx0-_c0p-Xxd7hfvyXr7tlrM14mBnMmkhppjnmdVYbhBa_PcCIFCIogq1TVanUJV86woC1NVItW2gtKClCkybnmZTokcck3wXRewVqfgjjpcFDB15aJuXNSVS7-rK5Kb9M754MS-3tlhUJ1x2PYtXEATlfXu34xfOHVvyQ |
| CitedBy_id | crossref_primary_10_1016_j_semcancer_2019_02_001 |
| ContentType | Journal Article |
| Copyright | 2008 American Society of Hematology |
| Copyright_xml | – notice: 2008 American Society of Hematology |
| DBID | 6I. AAFTH AAYXX CITATION |
| DOI | 10.1182/blood.V112.11.2717.2717 |
| DatabaseName | ScienceDirect Open Access Titles Elsevier:ScienceDirect:Open Access CrossRef |
| DatabaseTitle | CrossRef |
| DatabaseTitleList | CrossRef |
| DeliveryMethod | fulltext_linktorsrc |
| Discipline | Medicine Chemistry Biology Anatomy & Physiology |
| EISSN | 1528-0020 |
| EndPage | 2717 |
| ExternalDocumentID | 10_1182_blood_V112_11_2717_2717 S0006497119500118 |
| GroupedDBID | --- -~X .55 1CY 23N 2WC 34G 39C 4.4 53G 5GY 5RE 5VS 6I. 6J9 9M8 AAEDW AAFTH AAXUO ABOCM ABVKL ACGFO ADBBV AENEX AFFNX AFOSN AHPSJ ALMA_UNASSIGNED_HOLDINGS BAWUL BTFSW C1A CS3 DIK DU5 E3Z EBS EJD EX3 F5P FDB FRP GS5 GX1 IH2 K-O KQ8 L7B LSO MJL N4W N9A OK1 P2P R.V RHF RHI ROL SJN THE TR2 TWZ W2D W8F WH7 WOQ WOW X7M YHG YKV ZA5 ZGI 0R~ 0SF AALRI AAYXX ADVLN AITUG AKRWK AMRAJ CITATION H13 |
| ID | FETCH-LOGICAL-c1607-f1f2e665b8c2cedd66c44e47e14b3afeda31bf25898cbb43adb19d1773e02d293 |
| ISSN | 0006-4971 |
| IngestDate | Fri Aug 23 02:20:13 EDT 2024 Fri Feb 23 02:43:09 EST 2024 |
| IsDoiOpenAccess | true |
| IsOpenAccess | true |
| IsPeerReviewed | true |
| IsScholarly | true |
| Issue | 11 |
| Language | English |
| License | This article is made available under the Elsevier license. |
| LinkModel | OpenURL |
| MergedId | FETCHMERGED-LOGICAL-c1607-f1f2e665b8c2cedd66c44e47e14b3afeda31bf25898cbb43adb19d1773e02d293 |
| OpenAccessLink | https://dx.doi.org/10.1182/blood.V112.11.2717.2717 |
| PageCount | 1 |
| ParticipantIDs | crossref_primary_10_1182_blood_V112_11_2717_2717 elsevier_sciencedirect_doi_10_1182_blood_V112_11_2717_2717 |
| PublicationCentury | 2000 |
| PublicationDate | 2008-11-16 |
| PublicationDateYYYYMMDD | 2008-11-16 |
| PublicationDate_xml | – month: 11 year: 2008 text: 2008-11-16 day: 16 |
| PublicationDecade | 2000 |
| PublicationTitle | Blood |
| PublicationYear | 2008 |
| Publisher | Elsevier Inc |
| Publisher_xml | – name: Elsevier Inc |
| SSID | ssj0014325 |
| Score | 1.9471829 |
| Snippet | Aberrant methylation of CpG island of the promoter regions of genes is an important epigenetic mechanism, alternative to deletions or mutations, that cause the... Abstract Aberrant methylation of CpG island of the promoter regions of genes is an important epigenetic mechanism, alternative to deletions or mutations, that... |
| SourceID | crossref elsevier |
| SourceType | Aggregation Database Publisher |
| StartPage | 2717 |
| Title | Methylation of the PTEN Promoter Leads to PTEN Inactivation in Multiple Myeloma |
| URI | https://dx.doi.org/10.1182/blood.V112.11.2717.2717 |
| Volume | 112 |
| hasFullText | 1 |
| inHoldings | 1 |
| isFullTextHit | |
| isPrint | |
| link | http://sdu.summon.serialssolutions.com/2.0.0/link/0/eLvHCXMwtV3db9MwELe6IRgvE3SgjS_5AfGWkjhe4vBWtsIm1DFpHeItsmNHmhTSqWsf9t_vzh9pqoEAIV6s5OI47d0v54t9H4S8ZSpnYIXKSKg8izhM0ZGQWRJpsMZFGtd5XWDs8MlFfvZdHE_4ZDAIwX5r2n-VNNBA1hg5-xfS7gYFAhyDzKEFqUP7R3KfGmB90xmCaFeezyZnGBEAUjELzKiqbVoHSz5tMbLBrcvi2sc0OBhOb00z90o7bPo2vrK81aVXCxcL9hndWdu2U-_nspGOvroxmP2hu3Lp7xhj3WLjqh35DZAGY9zdNd8_rEQIDMlzgZJueSyEyGx4cOJ8iGXsHICM17KYFjtm8YYaTlgfb0lfq-YuvtPP0OH0vvYXmE3WevyPvsF4QBlh59F6gI3U2hfWIoPfhrVwMQR3izxgoLDQNfT49Eu3G8VT5iph-L_i_QThce9_8bCfWzk9y2X2hOz6Tw46dlh5SgamHZK9cSuX8x-39B21TsB2d2VIHn4MRztHoRTgkDyaeg-MPfK1hy86ryngiyKQaMAXtfiiy7kj9_FFr1oa8EU9vp6Ry0-T2dFJ5ItyRBXmIozqpGYmyw6VqFhltM6yinPDc5NwlcraaJkmqob3vxCVUjyVWiWFTvI8NTHTYFw-J9stgGyfUKV5lhXQU-sYhxCKF1rKXOoqM0ofHpA4MLG8drlXSvvNKlhp-V4i3-G8RJbb5oB8CMwuvQnpTMMSMPK7m1_8y80vyeP1O_GKbC8XK_OabN3o1RsLpju355DS |
| link.rule.ids | 315,782,786,27935,27936 |
| linkProvider | Flying Publisher |
| openUrl | ctx_ver=Z39.88-2004&ctx_enc=info%3Aofi%2Fenc%3AUTF-8&rfr_id=info%3Asid%2Fsummon.serialssolutions.com&rft_val_fmt=info%3Aofi%2Ffmt%3Akev%3Amtx%3Ajournal&rft.genre=article&rft.atitle=Methylation+of+the+PTEN+Promoter+Leads+to+PTEN+Inactivation+in+Multiple+Myeloma&rft.jtitle=Blood&rft.au=Piras%2C+Giovanna&rft.au=Pala%2C+Giuseppina&rft.au=Uras%2C+Antonella&rft.au=Calvisi%2C+Anna&rft.date=2008-11-16&rft.pub=Elsevier+Inc&rft.issn=0006-4971&rft.eissn=1528-0020&rft.volume=112&rft.issue=11&rft.spage=2717&rft.epage=2717&rft_id=info:doi/10.1182%2Fblood.V112.11.2717.2717&rft.externalDocID=S0006497119500118 |
| thumbnail_l | http://covers-cdn.summon.serialssolutions.com/index.aspx?isbn=/lc.gif&issn=0006-4971&client=summon |
| thumbnail_m | http://covers-cdn.summon.serialssolutions.com/index.aspx?isbn=/mc.gif&issn=0006-4971&client=summon |
| thumbnail_s | http://covers-cdn.summon.serialssolutions.com/index.aspx?isbn=/sc.gif&issn=0006-4971&client=summon |