| Literature DB >> 24666685 |
Maëliss Peigné1, Christine Decanter.
Abstract
Anti-Müllerian hormone (AMH) is a very sensitive indicator of the ovarian follicular content. Chemotherapeutic agents are notoriously ovariotoxic in that they damage follicles. The aim of this systematic review was to investigate the interest of serum AMH variations in determining the acute and long-term effects of chemotherapy on the ovarian reserve. According to the PRISMA guidelines, searches were conducted on PubMed for all English language articles until December 2013. Fifteen articles that focused on dynamic variations of AMH levels before and after chemotherapy were selected. Cancer patients have significantly lower AMH after chemotherapy than age-matched controls. Longitudinal studies of AMH variations before, during and after chemotherapy provide information about the degree of follicle loss for each patient according to different chemotherapy regimens. Different patterns of AMH levels during the ovarian recovery phase make it possible to discriminate between high and low gonadotoxic chemotherapy protocols. In addition, pretreatment AMH levels are shown to predict the long-term ovarian function after the end of treatment. These results may help to better understand the ovarian toxicity mechanisms of chemotherapy and to predict the degree of the ovarian follicle loss. Therefore, it can be useful for fertility preservation strategies, fertility counseling and future family planning.Entities:
Mesh:
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Year: 2014 PMID: 24666685 PMCID: PMC3987687 DOI: 10.1186/1477-7827-12-26
Source DB: PubMed Journal: Reprod Biol Endocrinol ISSN: 1477-7827 Impact factor: 5.211
Summary of studies with pre/post-treatment AMH measurements in young women undergoing chemotherapy (CT)
| Lutchman-Singh, 2007 [ | Breast | 22 | -AMH post-CT < AMH pre-CT |
| | | | -AMH pre-CT = AMH in age-matched controls |
| Lie Fong, 2008 [ | Haematological | 25 | -AMH post-CT < AMH pre-CT |
| | | | -AMH pre-CT < AMH in older controls |
| Aslam, 2011 [ | All types | 8 | -AMH post-CT < AMH pre-CT |
| | | | -AMH post-CT < AMH in age-matched controls with the same follow-up |
| Lawrenz, 2012 [ | Lymphoma | 38 | -AMH post-CT < AMH pre-CT |
| -AMH pre-CT < AMH in age-matched controls | |||
| -Number of retrieved oocyte for cryopreservervation in lymphoma < retrieved oocytes in women with breast cancer |
Summary of studies with longitudinal follow-up of serum AMH levels in young women undergoing chemotherapy (CT) for adult cancer
| Early stage breast cancer | 7 protocols all including alkylating agents | 41 (28–52) | Before CT, every 3 months during CT | 56 | -Significant fall of AMH levels 3 months after the start of CT. | |
| | | | | | | -Undetectable values of AMH in most patients at the end of CT. |
| | | | | | | -Different degrees of gonadotoxicity according to protocols. |
| Early stage breast cancer | Anthracycline, cyclophosphamide and taxane | 40 (21–51) | Before CT, 3 to 6 weeks post CT, 6 months and year post CT | 38 | -Undetectable values of AMH in most patients at the end of CT and one year post-CT. | |
| | | | | | | -Pre-CT AMH levels lower among women who became amenorrheic compared to those who resumed menses. |
| Lymphoma | Alkylating or non Alkylating regimens | 24 (18–32) | Before CT, 15 days after first cycle, 15 days before last cycle, every 3 months after CT until 1 year | 30 (17 non alkylating protocol, 13 alkylating protocol) | No difference between protocols regarding the depletion phase: | |
| -Acute fall of AMH as soon as 15 days after the start of CT. | ||||||
| -Undetectable values of AMH at the end of CT in both protocols. | ||||||
| Different recovery phases according to protocol: | ||||||
| -Very low or undetectable AMH levels in the alkylating group 1 year post-CT. | ||||||
| | | | | | | -Return to pre-treatment values of AMH as soon as the 6th month of follow-up in the non-alkylating group. |
| Lymphoma, Breast cancer, Ewing sarcoma | 7 different protocols | 30 (19–35) | Before CT, one week after each CT or every 2 weeks until 16 weeks of treatment, once a month until one year after first CT | 17 (13 alkylating protocol, 4 non alkylating protocol) | -Acute fall of AMH levels as soon as one week after the first cycle of CT. | |
| -Undetectable values of AMH in most patients at the end of CT. | ||||||
| | | | | | | -Significantly lower AMH one year after the end of CT in case of alkytlating protocols than in case of non alkylating ones. |
| Breast cancer | 3 different protocols all including alkylating agents | 37 (27–40) | Before CT, 6, 12, 36 and 52 weeks after first CT | 26 | -Significant fall of AMH levels 6 weeks after the start of CT. | |
| -Undetectable values of AMH in most patients at the end of CT. | ||||||
| | | | | | | -Undetectable AMH levels in all patient but one 52 weeks after first CT. |
| Early stage breast cancer | 7 protocols all including alkylating agents | 41 (28,6-52,7) | Before CT, 2,3,4 and 5 years post CT | 42 | -Lower serum AMH levels, 2–5 years after CT, than pretreatment ones. | |
| -Undetectable AMH in most women, 2–5 years post-CT. | ||||||
| | | | | | | -Pretreatment AMH level is strongly predictive of long term ovarian function after CT. |
| Different types of cancer | Different protocols | 26,1 (15 – 35,9) | Before CT, Every 3 month during and after treatment | 46 (33 alkylating protocol) | Difference between protocols regarding the depletion phase: | |
| -Significant fall of AMH levels 3 months after initiation of CT in alkylating and non-alkylating groups | ||||||
| -Lower AMH at the end of treatment with alkylating agents compared with unexposed participants | ||||||
| Different recovery phases according to protocol and to pretreatment AMH level: | ||||||
| -Rate of recovery of AMH 9 months after CT higher in non alkylating protocol than in alkylating protocol | ||||||
| | | | | | | -Rate of recovery of AMH 9 months after CT higher when pre-treatment AMH was >2 ng/ml than when it was ≤ 2 ng/m |
| Early stage breast cancer | 8 protocols, 7 including alkylating agents | 42,6 (23,3–52,5) | Before CT, after 1 or 2 cycles of CT, 1 and 2 years post CT | 59 | -Significant fall of AMH after 1 cycle of CT. | |
| -Undetectable values of AMH in most patients after 2 or more cycles of CT and at 1 year post CT. | ||||||
| | | | | | | -Pretreatment AMH level is strongly predictive of post CT ovarian function (menses) at 1 and 2 years post CT. |
| Breast cancer | 5 protocols all including alkylating agents except for 1 patient | 41 (25–50) | Before CT, 1 month post CT, 1 year post CT. | 27 | -Undetectable values of AMH in all patients 1 month post CT. | |
| -Undetectable AMH levels in most women 1 year post CT. |
Summary of studies with longitudinal follow-up of serum AMH levels in young girls undergoing chemotherapy (CT) for childhood cancer
| Different type of cancer | Different protocols (low/ medium/high gonadotoxic protocols) | 4,4 (0,3-15) | Before CT, after each CT course, between 2 and 12 months post CT, >12 months post CT | 22 (9 high gonadotoxic protocol, 13 medium or low gonadotoxic protocol) | No difference between protocols regarding the depletion phase: | |
| -Significant fall of AMH levels from the third cycle of CT in all protocols. | ||||||
| -Undetectable values of AMH in most patients at the end of CT. | ||||||
| Different recovery phases according to protocol: | ||||||
| -Very low or undetectable AMH levels in the high gonadotoxic group more than 12 months post CT. | ||||||
| | | | | | | -Return to pre-treatment AMH values as soon as the 6th month of follow-up in the medium/low group risk. |
| Different type of cancer | Different protocols | 9,5 (4,5-16,5) | Before CT, Every 3 month during and after CT | 34 (27 alkylating protocol) | No difference between protocols regarding the depletion phase: | |
| -Significant fall of AMH levels 3 months after initiation of CT. | ||||||
| Different recovery phases according to protocol: | ||||||
| -Very low or undetectable AMH levels in the group with irradiation below the diaphragm and/or stem cell transplantation 18 month post follow-up. | ||||||
| -Return to pre-treatment or higher AMH values as soon as the 15th month of follow-up in acute lymphatic leukemia group. |