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  1. Analyzed Page
  2. Matching Content Categories
  3. CMS
  4. Monthly Traffic Estimate
  5. How Does Link.springer.com Make Money
  6. Keywords
  7. Topics
  8. Questions
  9. Schema
  10. External Links
  11. Analytics And Tracking
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We are analyzing https://link.springer.com/article/10.1007/s00277-018-3311-z.

Title:
Bendamustine and rituximab (BR) versus dexamethasone, rituximab, and cyclophosphamide (DRC) in patients with Waldenström macroglobulinemia | Annals of Hematology
Description:
The treatment approaches for Waldenstrom macroglobulinemia (WM) are largely based upon information from single-arm phase II trials, without comparative data. We compared the efficacy of two commonly used regimens in routine practice (bendamustine-rituximab (BR) and dexamethasone, rituximab plus cyclophosphamide (DRC)) and evaluated their activity with respect to the patients’ MYD88L265P mutation status. Of 160 consecutive patients, 60 received BR (43 with relapsed/refractory WM) and 100 received DRC (50 had relapsed/refractory WM). In the treatment-naïve setting, overall response rate (ORR) was 93% with BR versus 96% with DRC (p = 0.55). Two-year progression-free survival (PFS) with BR and DRC was 88 and 61%, respectively (p = 0.07). In salvage setting, ORR was 95% with BR versus 87% with DRC, p = 0.45; median PFS with BR was 58 versus 32 months with DRC (2-year PFS was 66 versus 53%; p = 0.08). Median disease-specific survival was not reached with BR versus 166 months with DRC (p = 0.51). The time-to-event endpoints and depth of response were independent of the MYD88 mutation status. Grade ≥ 3 adverse events of both regimens were comparable. A trend for longer PFS was observed with BR although the regimens have comparable toxicities. The activity of BR and DRC appears to be unaffected by patients’ MYD88 mutation status.
Website Age:
28 years and 1 months (reg. 1997-05-29).

Matching Content Categories {📚}

  • Education
  • Science
  • Non-Profit & Charity

Content Management System {📝}

What CMS is link.springer.com built with?

Custom-built

No common CMS systems were detected on Link.springer.com, and no known web development framework was identified.

Traffic Estimate {📈}

What is the average monthly size of link.springer.com audience?

🌠 Phenomenal Traffic: 5M - 10M visitors per month


Based on our best estimate, this website will receive around 5,000,019 visitors per month in the current month.
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How Does Link.springer.com Make Money? {💸}

We see no obvious way the site makes money.

Earning money isn't the goal of every website; some are designed to offer support or promote social causes. People have different reasons for creating websites. This might be one such reason. Link.springer.com has a revenue plan, but it's either invisible or we haven't found it.

Keywords {🔍}

article, pubmed, macroglobulinemia, google, scholar, cas, rituximab, research, patients, waldenstroms, treon, versus, bendamustine, waldenstrom, received, institution, study, drc, treatment, lymphoma, oncol, data, myd, therapy, celgene, cyclophosphamide, ansell, kyle, kapoor, phase, castillo, clin, gertz, mayo, funding, kumar, morra, patterson, hunter, ibrutinib, usa, privacy, cookies, content, information, hematology, dexamethasone, waldenström, paludo, lacy,

Topics {✒️}

median disease-specific survival year progression-free survival month download article/chapter b-cell lymphoproliferative disorders relapsed indolent b-cell targeted genomic instability lymphoplasmacytic lymphoma access owen rg full article pdf mantle-cell lymphomas privacy choices/manage cookies myd88 mutation status waldenstrom macroglobulinemia/lymphoplasmacytic lymphomas front-line treatment regimens jama oncology 3 rummel mj received research funding phase iii study chronic lymphocytic leukemia article annals received research support clinical trial participation european economic area clinico-pathological profile tertiary care centre intermittent oral chlorambucil ohio lexi-comp adverse events v4 ethnic/racial minority ighv gene features institutional review board bristol-myers squibb leuk lymphoma 56 risk-adapted therapy conditions privacy policy consensus panel recommendations prashant kapoor year updated results article paludo mantle cell article log drug information handbook vith international workshop eighth international workshop 5th international workshop castillo jj accepting optional cookies clin lymphoma 5 chanan-khan aa common terminology criteria

Questions {❓}

  • Jimenez R, Zhang B, Joffe S, Nilsson M, Rivera L, Mutchler J, Lathan C, Paulk ME, Prigerson HG (2013) Clinical trial participation among ethnic/racial minority and majority patients with advanced cancer: what factors most influence enrollment?

Schema {🗺️}

WebPage:
      mainEntity:
         headline:Bendamustine and rituximab (BR) versus dexamethasone, rituximab, and cyclophosphamide (DRC) in patients with Waldenström macroglobulinemia
         description:The treatment approaches for Waldenstrom macroglobulinemia (WM) are largely based upon information from single-arm phase II trials, without comparative data. We compared the efficacy of two commonly used regimens in routine practice (bendamustine-rituximab (BR) and dexamethasone, rituximab plus cyclophosphamide (DRC)) and evaluated their activity with respect to the patients’ MYD88L265P mutation status. Of 160 consecutive patients, 60 received BR (43 with relapsed/refractory WM) and 100 received DRC (50 had relapsed/refractory WM). In the treatment-naïve setting, overall response rate (ORR) was 93% with BR versus 96% with DRC (p = 0.55). Two-year progression-free survival (PFS) with BR and DRC was 88 and 61%, respectively (p = 0.07). In salvage setting, ORR was 95% with BR versus 87% with DRC, p = 0.45; median PFS with BR was 58 versus 32 months with DRC (2-year PFS was 66 versus 53%; p = 0.08). Median disease-specific survival was not reached with BR versus 166 months with DRC (p = 0.51). The time-to-event endpoints and depth of response were independent of the MYD88 mutation status. Grade ≥ 3 adverse events of both regimens were comparable. A trend for longer PFS was observed with BR although the regimens have comparable toxicities. The activity of BR and DRC appears to be unaffected by patients’ MYD88 mutation status.
         datePublished:2018-04-03T00:00:00Z
         dateModified:2018-04-03T00:00:00Z
         pageStart:1417
         pageEnd:1425
         sameAs:https://doi.org/10.1007/s00277-018-3311-z
         keywords:
            MYD88
            Drug therapy
            Lymphoma
            Immunoglobulin M
            Lymphoplasmacytic lymphoma
            Hematology
            Oncology
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               1432-0584
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         author:
               name:Jonas Paludo
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               name:Craig B. Reeder
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                        name:Division of Hematology, Mayo Clinic, Scottsdale, USA
                        type:PostalAddress
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               name:Francis K. Buadi
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                        name:Division of Hematology, Mayo Clinic, Rochester, USA
                        type:PostalAddress
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               name:Angela Dispenzieri
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                        name:Division of Hematology, Mayo Clinic, Rochester, USA
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      headline:Bendamustine and rituximab (BR) versus dexamethasone, rituximab, and cyclophosphamide (DRC) in patients with Waldenström macroglobulinemia
      description:The treatment approaches for Waldenstrom macroglobulinemia (WM) are largely based upon information from single-arm phase II trials, without comparative data. We compared the efficacy of two commonly used regimens in routine practice (bendamustine-rituximab (BR) and dexamethasone, rituximab plus cyclophosphamide (DRC)) and evaluated their activity with respect to the patients’ MYD88L265P mutation status. Of 160 consecutive patients, 60 received BR (43 with relapsed/refractory WM) and 100 received DRC (50 had relapsed/refractory WM). In the treatment-naïve setting, overall response rate (ORR) was 93% with BR versus 96% with DRC (p = 0.55). Two-year progression-free survival (PFS) with BR and DRC was 88 and 61%, respectively (p = 0.07). In salvage setting, ORR was 95% with BR versus 87% with DRC, p = 0.45; median PFS with BR was 58 versus 32 months with DRC (2-year PFS was 66 versus 53%; p = 0.08). Median disease-specific survival was not reached with BR versus 166 months with DRC (p = 0.51). The time-to-event endpoints and depth of response were independent of the MYD88 mutation status. Grade ≥ 3 adverse events of both regimens were comparable. A trend for longer PFS was observed with BR although the regimens have comparable toxicities. The activity of BR and DRC appears to be unaffected by patients’ MYD88 mutation status.
      datePublished:2018-04-03T00:00:00Z
      dateModified:2018-04-03T00:00:00Z
      pageStart:1417
      pageEnd:1425
      sameAs:https://doi.org/10.1007/s00277-018-3311-z
      keywords:
         MYD88
         Drug therapy
         Lymphoma
         Immunoglobulin M
         Lymphoplasmacytic lymphoma
         Hematology
         Oncology
      image:
         https://media.springernature.com/lw1200/springer-static/image/art%3A10.1007%2Fs00277-018-3311-z/MediaObjects/277_2018_3311_Fig1_HTML.gif
         https://media.springernature.com/lw1200/springer-static/image/art%3A10.1007%2Fs00277-018-3311-z/MediaObjects/277_2018_3311_Fig2_HTML.gif
      isPartOf:
         name:Annals of Hematology
         issn:
            1432-0584
            0939-5555
         volumeNumber:97
         type:
            Periodical
            PublicationVolume
      publisher:
         name:Springer Berlin Heidelberg
         logo:
            url:https://www.springernature.com/app-sn/public/images/logo-springernature.png
            type:ImageObject
         type:Organization
      author:
            name:Jonas Paludo
            affiliation:
                  name:Mayo Clinic
                  address:
                     name:Division of Hematology, Mayo Clinic, Rochester, USA
                     type:PostalAddress
                  type:Organization
            type:Person
            name:Jithma P. Abeykoon
            affiliation:
                  name:Mayo Clinic
                  address:
                     name:Department of Internal Medicine, Mayo Clinic, Rochester, USA
                     type:PostalAddress
                  type:Organization
            type:Person
            name:Amanda Shreders
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                  name:Mayo Clinic
                  address:
                     name:Division of Hematology, Mayo Clinic, Jacksonville, USA
                     type:PostalAddress
                  type:Organization
            type:Person
            name:Stephen M. Ansell
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                  name:Mayo Clinic
                  address:
                     name:Division of Hematology, Mayo Clinic, Rochester, USA
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                  type:Organization
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            name:Shaji Kumar
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                  name:Mayo Clinic
                  address:
                     name:Division of Hematology, Mayo Clinic, Rochester, USA
                     type:PostalAddress
                  type:Organization
            type:Person
            name:Sikander Ailawadhi
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                  name:Mayo Clinic
                  address:
                     name:Division of Hematology, Mayo Clinic, Jacksonville, USA
                     type:PostalAddress
                  type:Organization
            type:Person
            name:Rebecca L. King
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                  name:Mayo Clinic
                  address:
                     name:Division of Hematopathology, Mayo Clinic, Rochester, USA
                     type:PostalAddress
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            type:Person
            name:Amber B. Koehler
            affiliation:
                  name:Mayo Clinic
                  address:
                     name:Division of Hematology, Mayo Clinic, Rochester, USA
                     type:PostalAddress
                  type:Organization
            type:Person
            name:Craig B. Reeder
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                  name:Mayo Clinic
                  address:
                     name:Division of Hematology, Mayo Clinic, Scottsdale, USA
                     type:PostalAddress
                  type:Organization
            type:Person
            name:Francis K. Buadi
            affiliation:
                  name:Mayo Clinic
                  address:
                     name:Division of Hematology, Mayo Clinic, Rochester, USA
                     type:PostalAddress
                  type:Organization
            type:Person
            name:Angela Dispenzieri
            affiliation:
                  name:Mayo Clinic
                  address:
                     name:Division of Hematology, Mayo Clinic, Rochester, USA
                     type:PostalAddress
                  type:Organization
            type:Person
            name:Martha Q. Lacy
            affiliation:
                  name:Mayo Clinic
                  address:
                     name:Division of Hematology, Mayo Clinic, Rochester, USA
                     type:PostalAddress
                  type:Organization
            type:Person
            name:David Dingli
            affiliation:
                  name:Mayo Clinic
                  address:
                     name:Division of Hematology, Mayo Clinic, Rochester, USA
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            name:Thomas E. Witzig
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                  name:Mayo Clinic
                  address:
                     name:Division of Hematology, Mayo Clinic, Rochester, USA
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            name:Ronald S. Go
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            name:Wilson I. Gonsalves
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            name:Nelson Leung
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            name:Yi Lin
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      name:Annals of Hematology
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      volumeNumber:97
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      name:Springer Berlin Heidelberg
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         name:Division of Hematopathology, Mayo Clinic, Rochester, USA
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