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Synthetics what blood tests and dosages

#1

I have made the decision that after my current break from pm i will book an appointment with my gp here in the uk for some blood tests and do a trial run (self medicating) of synthetics, hoping some of you girls can offer your advice on whether i have missed any tests in my list below?

Complete blood counts
Renal and liver function
Lipid and glucose metabolism
Serum testosterone and estradiol
Serum electrolytes particularly potassium
Prolactin levels (raised levels can be a sign of enlarged pituitary gland as a result of oestrogen treatment)
Bone mineral density (history of osteoporosis in the family)

And the starting dosages would be

2mg of estradiol sublingualy per day (1mg morning and evening)
100mg of spironolactone per day (50mg morning and evening)
5mg of finasteride per day (2.5mg morning and evening)

Followed by another serum test a month from starting then adjusting dosages as needed, i dont know whether i should increase the estradiol half way through the first month to 4mg or leave it at 2mg for the month?

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#2

That looks good. Any question about blood sugar levels? Adding a fasting glucose test and, optionally, an HbA1C test might be considered. Prostate health? PSA test would be advisable. I wonder if your doctor will approve the T and E tests without some justification.

What is your reason for a trial run on synthetics? Are you not sure about transitioning? If so, it might be best to stay with herbs and take it slow until you're more sure.

Your synthetics regimen is what I started out with a month ago. My blood testing had been done 3 months before that, so I was satisfied going ahead on my own. I'm very close to going under a doctor's supervision for my HRT at which point I will have my hormone levels measured and make the appropriate adjustments. On 2 mg/day I started to get night erections and feel anxious so I doubled it to 4 mg after a week. I've decided to add in 1000 mg/day of PM again along with the synthetics, That's the recommended dosage of PM for women.

Clara Smile
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#3

Thanks clara i will look into these other tests, i didnt know whether psa/prostate would be an issue with the proscar or not, why the trial run? well its not doubts i just wanted to know for sure that its not just the pm making me feel this way and i still feel the same way on the real e even though i have feelings going back as far as i can remember (certainly when i was 5), im going to be upfront with my gp about it all even what im taking and dosages, national health service here and in theory they have a duty of care to treat or if they have a big issue with it pass you on to someone else to treat, i have spoken to the nearest gender clinic already but it seems a slow drawn out process just to get seen and then at least 3 months before you see any hormones so i figured i would go this route in the meantime while i wait, the good news it seems it things in the uk have changed for the better and now facial hair removal and speach therapy are covered by the nhs Smile
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#4

By the way clara what dosage of spiro where you on when you went from 2mg to 4mg of eostradiol as i seem to recall you where keeping your spiro dosage down, reason for asking was as i understand it its preferable to use spiro in order to keep eostradiol dosage as low as possible, granted i know 2mg even sublingually is low

Something else i should have asked about was serum levels, the endocrine society's guide suggests

"Serum estradiol should be maintained at the mean daily level for pre-menopausal women (<200 pg/ml), and the serum testosterone level should be in the female range (<55 ng/dl)."

Does this sound about right? maybe those of you being monitored could let me know
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#5

Yes, Bobie, I ramped up the Spiro, too, from 50 to 100 mg. I did that mainly to see how it affects my blood pressure which is rather low. It turns out it didn't have an effect on my BP at all.

You don't need to take a T-blocker, like Spiro, to feminize. The body will cut the production of T automatically when you raise the amount of E in your system in order to maintain a certain combined level of sex hormone (T + E). The thing is, whatever T your body does produce is going to have a masculinizing effect on your body, as well as help keep your sex drive going which may be something you want for the sake of your marriage, etc.

But, if your goal is to feminize yourself as much as possible, as fast as possible, and you don't care if your sex drive drops to zero, you'll want to take a T-blocker to counter the effects of T.

As long as my BP is not affected, I plan to ramp up to 200 mg of Spiro over the next month. I'd like my T level to fall into the range of a typical woman.

Clara Smile

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#6

(15-06-2014, 09:47 PM)ClaraKay Wrote:  That looks good. Any question about blood sugar levels? Adding a fasting glucose test and, optionally, an HbA1C test might be considered. Prostate health? PSA test would be advisable. I wonder if your doctor will approve the T and E tests without some justification.

What is your reason for a trial run on synthetics? Are you not sure about transitioning? If so, it might be best to stay with herbs and take it slow until you're more sure.

Your synthetics regimen is what I started out with a month ago. My blood testing had been done 3 months before that, so I was satisfied going ahead on my own. I'm very close to going under a doctor's supervision for my HRT at which point I will have my hormone levels measured and make the appropriate adjustments. On 2 mg/day I started to get night erections and feel anxious so I doubled it to 4 mg after a week. I've decided to add in 1000 mg/day of PM again along with the synthetics, That's the recommended dosage of PM for women.

Clara Smile

Clara, how did the mix of E and PM go? , I thought I had read in another thread about weaker E blocking or locking the receptors so the stronger E would not be used, would this be the case here too ?? Or does E and PM co_exist just fine?
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#7

(18-06-2014, 06:02 PM)Janet doe Wrote:  Clara, how did the mix of E and PM go? , I thought I had read in another thread about weaker E blocking or locking the receptors so the stronger E would not be used, would this be the case here too ?? Or does E and PM co_exist just fine?

Hi Janet,

I do believe that PM (miroestrol) competes with estradiol for estrogen receptors in breast tissue. That's good for lowering the risk of breast cancer. But, the reason that I've added 1000 mg of PM back into my regimen was for other benefits of PM. I liked that PM was helping to ease morning joint stiffness which returned when I went off PM. On the other hand, my nipples become 'hard' and my areolas dark on the PM, which my DW is not particularly crazy about, and they do tend to show extremely well through a single layer of clothing Blush. I'm exploring the possibility of finding another herb that helps with joint health so that I can drop the PM. I'm not that concerned about breast cancer because there are no instances of it in my family background. I also don't like the fact that the phyto-estrogen from PM doesn't show up in the standard estrogen tests that my endo will be calling for to help establish an optimal sex hormone balance.

Don't take these comments as a shift in my attitude about the benefits of herbal HRT. I do NOT regret having used herbs the first 7 months of my feminization program. I needed that time to really come to know myself better, and to grow into my true gender identity. I highly recommend herbal HRT for those who are in the exploratory phase of their gender conundrum.

Hugs,

Clara Smile
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#8

(15-06-2014, 09:20 PM)bobie Wrote:  I have made the decision that after my current break from pm i will book an appointment with my gp here in the uk for some blood tests and do a trial run (self medicating) of synthetics, hoping some of you girls can offer your advice on whether i have missed any tests in my list below?

Complete blood counts
Renal and liver function
Lipid and glucose metabolism
Serum testosterone and estradiol
Serum electrolytes particularly potassium
Prolactin levels (raised levels can be a sign of enlarged pituitary gland as a result of oestrogen treatment)
Bone mineral density (history of osteoporosis in the family)

And the starting dosages would be

2mg of estradiol sublingualy per day (1mg morning and evening)
100mg of spironolactone per day (50mg morning and evening)
5mg of finasteride per day (2.5mg morning and evening)

Followed by another serum test a month from starting then adjusting dosages as needed, i dont know whether i should increase the estradiol half way through the first month to 4mg or leave it at 2mg for the month?

Bobie,

Here's Dr. Anne Lawerence suggested regime,



Feminizing Hormone Regimens


I receive frequent inquiries from transgender persons who want my advice concerning feminizing hormone regimens. These individuals may wish to educate their physicians, or may plan to self-administer hormones without medical supervision. Sometimes I also receive inquiries from physicians directly.
Naturally, I believe that taking hormones under medical supervision is by far the best and safest course. But I also believe that transsexual women who decide for whatever reason to take hormones without medical supervision ought to have as much information as possible to guide them. Here are my thoughts:

Estrogen is the most important part of any feminizing regimen. Some typical initial estrogen dosages for preoperative transsexual women who have not undergone SRS or orchiectomy (castration) are as follows:

Oral estrogens:
estradiol (e.g., Estrace® or Estrofem®), 6-8 mg daily; OR

estradiol valerate (e.g., Progynova®), 6-8 mg daily; OR

conjugated equine estrogens (e.g., Premarin®), 5 mg daily; OR

ethinyl estradiol (e.g., Estinyl®), 100 mcg (0.1 mg) daily (NOT RECOMMENDED); OR

Transdermal estrogen:

estradiol (e.g., Vivelle-Dot®, Estraderm®, Climara®, etc.), two 0.1 mg patches, applied simultaneously, changed per manufacturer's recommended schedule (see note below); OR

Injectable (intramuscular) estrogen (NOT RECOMMENDED):

estradiol valerate (e.g., Delestrogen®), 20 mg IM every two weeks.
Occasionally half the suggested dosage may be sufficient. Sometimes the dosage will need to be increased, rarely even doubled. Beyond a certain point, larger dosages will not increase tissue response, but will only cause more side effects.
Oral estrogens are most commonly used, and are typically very satisfactory. Among the oral preparations, I prefer estradiol (or estradiol valerate, which is virtually identical). Estradiol is very inexpensive, and has low hepatic toxicity. Most clinical laboratories can perform estradiol blood levels; it is more difficult to obtain meaningful measurements of blood levels with conjugated equine estrogen or with ethinyl estradiol. Estradiol is also produced synthetically, without cruelty to animals. This is not the case with conjugated equine estrogen (Premarin®), which is prepared from the urine of pregnant mares.

Estradiol tablets can be taken sublingually (placed under the tongue to dissolve) instead of being swallowed. This may reduce possible liver toxicity, because with sublingual administration, much of the medication is absorbed directly into the blood stream, rather than being metabolized by the liver after first passing through the digestive tract. Less metabolism is also likely to result in higher levels of estradiol itself, and lower levels of its less-active metabolites, estrone and estriol. Micronized estradiol tablets are specifically designed for either oral or sublingual use and dissolve quickly under the tongue without an unpleasant taste.

Premarin® is by far the most expensive oral preparation. One of its few advantages is its relative potency, which is notably higher than estradiol on a milligram-per-milligram basis. This is because some of the equine estrogens in Premarin, especially equilin, have higher biologic potency than the estrogens normally found in humans.

Ethinyl estradiol is a chemically-modified form of natural estradiol. The ethinyl substitution results in a longer duration of action, and greatly increased potency. Consequently, typical milligram dosages of ethinyl estradiol are about one-fiftieth of typical milligram doses of estradiol. This is a preparation I do not recommend, due to its association with thromboembolic complications; see Toorians et al. (2003). Venous thrombosis and changes of hemostatic variables during cross-sex hormone treatment in transsexual people. Journal of Clinical Endocrinology and Metabolism, 88, 5723-5729.

I think that taking 81 mg of aspirin daily is a good precaution for persons taking oral estrogens, assuming no contraindication to aspirin exists.

Transdermal estrogen causes less clotting tendency than oral estrogen, which is possibly important to some patients. However, transdermal preparations are more expensive, and skin reactions to the adhesives employed are not uncommon. I recommend transdermal estrogen for most patients over the age of 40, to patients with risk factors such as cigarette smoking, and to patients with a personal or family history of cardiovascular disease. Transdermal patches should be changed according to the manufacturer's recommended schedule: twice weekly for most patches, weekly for Climara®.

Injectable estrogen may cause less clotting tendency than oral estrogen and it is less expensive than transdermal estrogen. However, it requires the use of needles and syringes, and the ability to perform injections; it has a greater tendency to increase serum prolactin levels; and it is often associated with inadvertent or deliberate overdosage. Contrary to the belief of many consumers, there is no credible evidence that injectable estradiol produces superior feminization. I do not recommend the use of injectable estrogen and I no longer prescribe it in my practice.

If you have access to laboratory testing, a serum estradiol level of about 125-200 pg/ml – about one-third to one-half the normal female mid-cycle peak – is often considered ideal, at least for the first two years or so of feminizing therapy. It is not necessary or desirable to "cycle" estrogen, or any other medication, in an attempt to mimic the normal female menstrual cycle.

Besides providing estrogen, a hormone regimen should also reduce testosterone to normal female levels. This usually requires adding an anti-androgen.

In persons who have not had an orchiectomy, reducing testosterone levels is also a concern. Although the desired reduction in testosterone can theoretically be accomplished with estrogen alone, the dosage required is usually in excess of what is needed for feminization. Adding an anti-androgen allows lower dosages of estrogen to be used; this is usually highly desirable. Typical dosages of anti-androgens are as follows:

Oral anti-androgens:
spironolactone (e.g., Aldactone®), 100-300 mg daily in divided doses; OR

cyproterone acetate (e.g., Androcur®), 100-150 mg daily.

Sometimes 100 mg of spironolactone may be sufficient, but 200–300 mg is a more typical dose. The Vancouver group uses up to 600 mg daily, apparently without problems. Spironolactone is fairly inexpensive, is readily available, and is usually quite well tolerated. In my opinion, it should be regarded as the anti-androgen of choice for most patients. Cyproterone is actually a progestin (see below), but it is used primarily for its anti-androgenic effects and only secondarily for its progestational effects. It is not available in the US, but is popular elsewhere. One disadvantage of cyproterone is that it counteracts some of the desirable effects of estrogen on blood lipids. Cyproterone, when used in combination with estrogen, may also share some of the increased risks associated with the synthetic progestin medroxyprogesterone when so used (see below).
If you have access to laboratory testing, a serum testosterone level within the normal female range – about 5-85 ng/dl for total testosterone, or 0.1–2.2 pg/ml for free testosterone – is usually considered ideal. Within the female normal range, lower numbers are not necessarily better.

Progestins (progesterone and synthetics) are sometimes added to a hormone regimen. I consider them unnecessary for most patients.

Progestins are most often given in an attempt to increase breast development. Based on limited anecdotal evidence, I think that improved breast development sometimes can occur, but that the effects are usually not very significant. Progestins can also inhibit testosterone production, and are sometimes used for this purpose. I consider progesterone and other progestins to be unnecessary for most patients, and I prescribe them only rarely. If you decide to take them, here are some typical dosages:

Oral progestins:
medroxyprogesterone (e.g., Provera®), 5-10 mg daily; OR

micronized progesterone (e.g., Prometrium®), 100 mg twice daily; OR

Injectable (intramuscular) progestins:

medroxyprogesterone (e.g., Depo-Provera®), 50 mg every two weeks; OR

progesterone in oil, 50 mg every two weeks.

Oral medroxyprogesterone, the most commonly used product, is very inexpensive, but it has the disadvantage of counteracting some of the beneficial effects of estrogen on blood lipids. Some people find that it causes depression or mental irritability. The recently published Women’s Health Initiative study has also documented an increased incidence of adverse complications in women taking medroxyprogesterone in combination with conjugated estrogens for hormone replacement; this increased incidence of adverse complications was not found with conjugated estrogens alone. Micronized progesterone is a reasonable alternative in those who want to take a progestin. It does not counteract the beneficial effects of estrogen on blood lipids. But micronized progesterone is more expensive, and is often harder to obtain. When taken by mouth, it is partially metabolized to 5-alpha and 5-beta pregnenolone; these metabolites can act as natural tranquilizers, and may promote sleep. This effect may be desirable in patients who suffer from anxiety or insomnia.

After orchiectomy (castration) or SRS, dosages can be reduced. Following SRS, anti-androgens can be discontinued, and estrogen dosage can usually be decreased to one-half or one-quarter of the pre-op dosage, i.e.:

Oral estrogens:
estradiol (e.g., Estrace® or Estrofem®), 1-2 mg daily; OR

estradiol valerate (e.g., Progynova®), 1-2 mg daily; OR

conjugated equine estrogens (e.g., Premarin®), 0.625-1.25 mg daily; OR

ethinyl estradiol (e.g., Estinyl®), 20-50 mcg (0.02-0.05 mg) daily; OR

Transdermal estrogen:

estradiol (e.g., Climara®, Estraderm®, or equivalent), 0.05-0.1 mg, changed per manufacturer's recommended schedule; OR

Injectable (intramuscular) estrogen:

estradiol valerate (e.g., Delestrogen®), 5-10 mg IM every two weeks.
(Injectable estradiol is rarely used after orchiectomy or SRS because the doses required are so small.)

© 2004 by Anne A. Lawrence, M.D., Ph.D. All rights reserved.

http://annelawrence.com/regimens.html



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#9

Thank you lotus the information is greatly appreciated and sorry if i was the cause of the recent discussion (herbal versus synthetics), i hope if nothing else people can see from this thread that i am trying to do things sensibly under a doctors supervision even if not going through official channels at this time

I do have one question and that is as my body is now used to pm if aiming for a dosage of 4mg sublingually prior to the first round of tests with e in my system would i need to start off at 2mg and work up to 4mg or would i be able to start off at 4mg?

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#10

(18-06-2014, 08:45 PM)bobie Wrote:  I do have one question and that is as my body is now used to pm if aiming for a dosage of 4mg sublingually prior to the first round of tests with e in my system would i need to start off at 2mg and work up to 4mg or would i be able to start off at 4mg?

That's what I did, just to be safe. 2mg is a very low dosage, so I'm not sure I needed to be so cautious, but I like to ramp up on any new substance I start taking, just in case I have a bad reaction.

Clara Smile
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