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  1. #1
    fabry is offline Senior Member
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    10mg nolva + 25mg proviron in sust-tren-winny cycle, ok?

    is this combo ok to fight sides from different gear (sust 12 wks and tren /winny and of cycle).
    some say letro, but its difficult to get it here in italy, even if in liquid form...
    so, if the stuff i have, nolva and proviron , will be ok, ill just use that...
    i aslo have ldex, but not sure about how much left...
    thanks

  2. #2
    BajanBastard is offline VET Retired
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    I would aviod the nolva on a cycle with tren . 50mg of proviron maybe?

  3. #3
    fabry is offline Senior Member
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    why not nolva with tren ?

  4. #4
    BajanBastard is offline VET Retired
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    Nolva increases the chances of getting tren gyno.

  5. #5
    fabry is offline Senior Member
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    ah, sh!t didnt know that... so maybe letro? and just letro?

  6. #6
    BajanBastard is offline VET Retired
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    Yeah letro would be ideal.

  7. #7
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    damian is offline Associate Member
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    Quote Originally Posted by big k.l.g
    Nolva increases the chances of getting tren gyno.

    i would like to see some hard evidence on that

  8. #8
    BajanBastard is offline VET Retired
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    Gynecol Oncol. 1999 Mar;72(3):331-6.

    Effects of tamoxifen on steroid hormone receptors and hormone concentration and the results of DNA analysis by flow cytometry in endometrial carcinoma.

    Nola M, Jukic S, Ilic-Forko J, Babic D, Uzarevic B, Petrovecki M, Suchanek E, Skrablin S, Dotlic S, Marusic M.

    Department of Gynecology and Obstetrics, University Hospital and School of Medicine, Zagreb, Croatia.

    OBJECTIVES: Tamoxifen is a nonsteroidal triphenylethylene derivate with a predominant antiestrogen activity, used in the endocrine treatment of breast and endometrial cancer. It is not known which endometrial carcinomas will respond favorably to tamoxifen and which ones will not. The aim of this study was to find out whether tamoxifen has an effect on hormone steroid receptors, hormone concentration, DNA content, and proliferative activity in endometrial cancer and to correlate the tamoxifen-induced changes with pathologic parameters such as clinical stage, tumor differentiation, depth of invasion, and histologic type. METHODS: Thirty postmenopausal women with endometrial carcinoma were treated with 30 mg of tamoxifen daily for 7-10 days after curettage. Steroid hormone receptors (estrogen and progesterone receptors), levels of follicle-stimulating hormone, luteinizing hormone, prolactin, estradiol, progesterone, testosterone , dehydroepiandrosterone sulfate, sex hormone binding globulin, and DNA ploidy and proliferative activity were determined before and after therapy. The patients were also divided into favorable and unfavorable prognosis groups according to classical histological parameters. The patients in the favorable group consisted of patients with stage I disease, well and moderately differentiated tumors, favorable histologic type, and a depth of myometrial invasion of less than (1/3). The patients with only one of the unfavorable parameters (clinical stage II or III, poorly differentiated tumors, unfavorable histologic types, and deeper invasion of myometrium) were included in the unfavorable prognosis group. RESULTS: After the treatment, there was a net increase in the progesterone receptors and sex hormone binding globulin and a significant decrease in the estrogen receptors. The increase in progesterone receptors and decrease in estrogen receptors occurred in the patient group with favorable prognosis regarding histologic type, degree of differentiation, and clinical stage, but also in the unfavorable prognosis group regarding the depth of myometrial invasion. Statistically significant decrease in the follicle-stimulating hormone concentration was observed in the groups with favorable prognosis regarding histologic type, depth of myometrial invasion, and grade of differentiation. Concentration of sex hormone binding globulin was significantly increased in groups with favorable prognosis if histologic type and grade of differentiation were taken into account. On the other hand, there was a significant decrease in the concentration of luteinizing hormone in the group with unfavorable histologic type and also a decrease in progesterone concentration in patients with unfavorable prognosis regarding the grade of differentiation. There was no statistical significance either in the concentrations of other hormones measured or in the DNA analysis by flow cytometry. CONCLUSIONS: Our results revealed that tamoxifen can increase progesterone receptors and decrease estrogen receptors in endometrial cancer. The effect was most pronounced in tumors with favorable clinicopathologic parameters. We conclude that tamoxifen therapy can induce progesterone receptor synthesis even in tumors with low initial progesterone receptor levels, making such tumors potentially responsive to additional hormonal therapy with progesterone.
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    Trenbolone has a binding affinity to the progesterone receptor (PgR) of about 60% if the actual progesterone hormone and one of it metabolites has a higher binding affinity to the PgR than progesterone itself. With nolva upregulating the PgR your chances of getting gynecomastia are increased.

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