Author: Mahmoud,Yasmin Ahmed ./ Title: Assessment of Minimal Residual Disease in Multiple Myeloma patients undergoing Autologous Stem Cell Transplant detected using Multiparameter Flow Cytometry/

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العنوان

Assessment of Minimal Residual Disease in Multiple Myeloma patients undergoing Autologous Stem Cell Transplant detected using Multiparameter Flow Cytometry/

الناشر

Faculty of Medicine

المؤلف

Mahmoud,Yasmin Ahmed .

هيئة الاعداد

باحث / Yasmin Ahmed Mahmoud

مشرف / Nevine Nabil Mostafa

مشرف / Walaa Ali El Salakawy

مشرف / Haitham Mohammed Mohammed Abdelbary

مشرف / Rania Abd El Monem Radwan

مشرف / Rasha Kamel Fathy

الموضوع

minimal residual disease, flow cytometry, autologous stem cell transplant

تاريخ النشر

2020

عدد الصفحات

183.p;

اللغة

الإنجليزية

الدرجة

الدكتوراه

التخصص

الطب الباطني

تاريخ الإجازة

1/1/2020

مكان الإجازة

جامعة عين شمس - كلية الطب - Internal Medicine

الفهرس

Only 14 pages are availabe for public view

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Abstract

BACKGROUND: Multiple Myeloma (MM) is still considered an incurable relapsing disease, despite major advances in multidrug combinations, incorporation of autologous transplant and achieving higher rates of CR. This suggests persistent presence of residual disease, not detected by current techniques. Minimal residual disease (MRD) monitoring by multiparameter flow cytometry (MFC) is a powerful tool to quantitatively measure residual disease and allow tailoring of the management plan on individual basis.
AIM: To assess the value of MRD by MFC in determining the efficacy of treatment, monitoring depth of remission and predicting impending relapse.
PATIENTS AND METHODS: We included 33MM patients, who were candidates for ASCT in this prospective study. MFC (with a 0.01% limit of detection) on a BM aspirate obtained before transplant and at day 100 post-transplant, was used to measure MRD for all patients. Patients were then later assessed for progression 1-year post-transplant.
RESULTS: MRD status at 100 days post-transplant was strongly related to the risk of 1-year post-transplant progression (p-value 0.001), and by using a ROC curve, we found that MRD (%) at 100 days post-transplant can predict progression after 1 year with a best cutoff value > 0.04 achieving a 75% sensitivity and 81.2% specificity. On dividing the patients according to their MRD status before and after transplant, group 3 who were MRD positive pre- and post-transplant, had a high risk of progression 1-year post-transplant (p-value 0.003). The use of bortezomib-based regimens resulted in a deeper response and a more negative MRD pre-transplant (p-value 0.01), that was maintained post-transplant. Also, ASCT resulted in the development of deeper remission (p-value 0.004) and more MRD negativity (p-value 0.02).
CONCLUSION: we recommend the use of MRD by MFC as a powerful prognostic tool, that should be incorporated in routine myeloma workup