Raadpleeg ook de literatuurlijsten niet-toxische middelen en behandelingen van arts-bioloog drs. Engelbert Valstar specifiek bij borstkanker.

Zie ook in gerelateerde artikelen.

18 oktober 2023: Bron: Clinical Breast Cancer

Uit een retrospectieve studie bij totaal 224 patiënten met in de botten uitgezaaide borstkanker en die minimaal twee jaar hun borstkanker overleefden, blijkt dat het niet zoveel uitmaakt of de borstkankerpatiënten Zometa - Zoledroniczuur of Denosumab krijgen als botversterker. Beide medicijnen hadden een positief effect in het verminderen van botgerelateerde voorvallen zoals botbreuken en botschade door behandelingen op het meetpunt van 2 jaar.

In deze studie bij totaal 224 patiënten met in de botten uitgezaaide borstkanker die uitgevoerd werd in het MD Anderson ziekenhuis in Houston waren de patiënten ingedeeld in drie groepen. (1) 52 patiënten die alleen Zometa - Zoledroniczuur kregen; (2) 137 patiënten die alleen Denosumab kregen; (3) 35 patiënten die zowel ZA als denosumab kregen.

Hoewel niet statistisch significant bleek Denosumab minder botproblemen te geven in vergelijking met Zometa Zometa - Zoledroniczuur, Het totaal aantal botvoorvallen (SRE's) bedroeg 21,2% van de patiënten die alleen Zometa Zometa - Zoledroniczuur kregen, 8,8% van degenen die alleen Denosumab kregen en 20% van de patiënten die beide botversterkers kregen. 

Welke botproblemen (SRE's) zich voordeden zie onderstaande grafiek, waarbij het totale aantal wel een verschil liet zien maar uitgesplitst bij de ene botversterker weer wat meer dan bij de andere en min of meer gelijk verdeeld over alle drie de groepen. 

Table 2 Skeletal-related events and BTT-associated harms
EventZolendronic AcidDenosumabBoth
Total SREs 10/52 (19.2%) 12/137 (8.9%) 7/35 (20%)
Pathologic fracture 4/52 (7.7%) 10/137 (7.3%) 3/35 (8.6%)
Compression fracture 4/52 (7.7%) 1/137 (0.7%) 2/35 (5.7%)
Palliative radiation 3/52 (5.8%) 1/137 (0.7%) 2/35 (5.7%)
Total BTT harms 3/52 (5.8%) 16/137 (11.7%) 5/35 (14.3%)
Osteonecrosis 3/52 (5.8%) 15/137 (10.9%) 4/35 (11.4%)
Atypical femur fracture 0/52 (05) 1/137 (0.7%) 1/35 (2.9%)
Abbreviations: SRE = skeletal-related events; BTT = bone-targeted therapy.

Zie ook Tables 3 en 4  

Practische punten voor gebruik van botversterkers in de klinische praktijk:
  • Botversterkers (BTT), waaronder zoledroninezuur (ZA) en denosumab, verlagen het risico op skeletgerelateerde voorvallen (SRE's) bij patiënten met gemetastaseerde borstkanker (MBC) en botmetastasen.
  • Er ontbreken gegevens over de aantallen SRE's en door borstversterkers geassocieerde schade bij patiënten met uitgezaaide borstkanker (MBC) en botuitzaaiingen na twee jaar behandeling.
  • In dit retrospectieve onderzoek werden 224 patiënten met MBC en botmetastasen geanalyseerd die meer dan twee jaar lang werden behandeld, onderverdeeld in drie BTT-patronen: alleen ZA, alleen denosumab en zowel ZA als denosumab.
  • Deze studie vond geen verschil in totale SRE's en door botversterkers geassocieerde schade tussen deze drie behandelingsgroepen; patiënten die alleen denosumab kregen, hadden echter een verminderde onderdrukking van het ruggenmerg.
  • De resultaten ondersteunen de flexibiliteit wanneer een oncoloog een middel en een frequentie voor botversterkers selecteert die langer duren dan twee jaar.

Het volledige studierapport is gratis in te zien. Klik op de titel van het abstract:

Bone-Targeted Therapy Regimen and Skeletal-Related Events in Patients Surviving Longer Than 2 Years With Metastatic Breast Cancer and Bone Metastasis

Published:August 29, 2023DOI:https://doi.org/10.1016/j.clbc.2023.08.008

Abstract

Background

Bone-targeted therapy (BTT) including zoledronic acid (ZA) and denosumab decreases the risk of skeletal-related events (SREs) in patients with metastatic breast cancer (MBC) and bone metastasis. The impacts from prolonged BTT on SREs and BTT-associated harms are unknown and are becoming important to understand as these patients survive for longer periods.

Methods and Materials

We conducted a retrospective study of 224 patients with MBC and bone metastasis who survived for more than 2 years after diagnosis and received treatment at our institution between 2016 and 2021. We defined 3 BTT patterns: (1) ZA only, (2) denosumab only, (3) both ZA and denosumab. The association between these BTT patterns and SREs and harms was assessed using Fisher exact test and logistic regression.

Results

Rates of SREs overall were 21.2% of patients given ZA only, 8.8% of those given denosumab only, and 20% of those given both, without statistically significant differences (p = .32). However, those treated with denosumab only had significantly fewer compression fractures (0.7%) (p = .02). BTT-associated harm was observed in 5.8% of the ZA-only group, 11.7% of the denosumab-only group, and 14.3% of the group given both, without statistically significant differences (p = .37).

Conclusion

Oncologists may have increased flexibility regarding the frequency of administration of BTT along with their choice of agent. Our study showed no significant difference in the prevention of overall SRE or development of BTT-associated harms between the BTT regimens evaluated.

Clinical Practice Points

  • Bone-targeted therapy (BTT) agents including zoledronic acid (ZA) and denosumab decrease the risk of skeletal-related events (SREs) in patients with metastatic breast cancer (MBC) and bone metastasis.
  • Data are lacking regarding the rates of SREs and BTT-associated harms in patients with MBC and bone metastasis beyond 2 years of treatment.
  • This retrospective study analyzed 224 patients with MBC and bone metastasis who received treatment for more than 2 years, categorized into 3 BTT patterns: ZA only, denosumab only, and both ZA and denosumab.
  • Thiis study found no difference in overall SREs and BTT-associated harms between these 3 treatment groups; however, patients who received denosumab only did have reduced rates of spinal cord compression.
  • Results supports flexibility when an oncologist selects an agent and a frequency for BTT regimens extending beyond 2 years.

Data Availability Statement

The data that support the findings of this study are available by request from the corresponding author.

Previous Presentations

The abstract of this study was presented as an online abstract at the ASCO 2022 meeting.

Ethics Statement

The University of Texas MD Anderson Cancer Center institutional review board approved this investigation (IRB #2021-0541, date of approval: 6/1/2021). A waiver of informed consent was granted by the institutional review board.

Acknowledgments

This research was supported by the National Cancer Institute through The University of Texas MD Anderson's Cancer Center Support Grant (P30CA016672). We thank Ashli Nguyen-Villarreal, Associate Scientific Editor, and Sarah Bronson, Scientific Editor, in the Research Medical Library at The University of Texas MD Anderson Cancer Center, for editing this article.

Disclosure

All authors declare no conflict of interest.

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Article info

Publication history

Published online: August 29, 2023
Accepted: August 27, 2023
Received in revised form: August 2, 2023
Received: May 22, 2023

Publication stage

In Press Journal Pre-Proof

Identification

DOI: https://doi.org/10.1016/j.clbc.2023.08.008

Copyright

© 2023 Elsevier Inc. All rights reserved.

ScienceDirect

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Tables

denosumab, Zometa, zoledroninezuur, uitgezaaide borstkanker, botproblemen, botuitzaaiingen


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