Contraceptive methods, what do you use?

[Negus]

from a balikbayan. I don't know where to source them locally..

[dark_akatsuke24]

Beyond the Condom: The Future of Male Contraception


Men have long had a limited choice of contraceptive methods: abstinence, withdrawal, condoms and vasectomy. With about three million unplanned or unwanted pregnancies a year in the U.S. alone, however, there is clearly room for more effective methods.

Male contraceptive research today pursues the ideal of birth control that is safe, long-acting but readily reversible, virtually free of side effects and applied sometime other than just before ***. Such a method would also reduce the spread of ***ually transmitted diseases and be inexpensive. No product under investigation can meet all these criteria, but several methods could potentially meet many of them.

Although research has progressed, male physiology conspires against an easy solution. Every day a man produces tens of millions of sperm, making their elimination or inactivation a daunting task. A woman, in contrast, usually releases only one egg per ovulation cycle. What is more, production of sperm in the testes and their later maturation in the adjoining ducts of the epididymis, where they become capable of fertilizing an egg, take about 75 days. Thus, no intervention in the testes, even if it immediately suppresses the making of sperm, will be contraceptive for almost two and a half months. Conversely, it takes an equal amount of time to return to fertility after stopping use of the contraceptive.

Given these inherent challenges, wholly new types of male contraceptives may not arrive for at least five to 10 years. This lag may seem surprising, but development of any new contraceptive technology takes 10 to 20 years. In the interim, new approaches to conventional contraceptives, including better condoms, may help meet the demand for improvements in male birth control.

[dark_akatsuke24]

New Strategies

Basic research on sperm formation may lead to an array of new contraceptive strategies. In sperm development the spermatogonia, the cellular precursor of sperm, arise from undifferentiated stem cells found in thin, coiled structures in the testes, the seminiferous tubules. When the stem cells divide, some of their progeny develop into the spermatogonia, which eventually become sperm; the rest remain as stem cells, thereby replenishing the supply of these cells.

Once these events take place, the sperm-cells-to-be move slowly to a central part of the seminiferous tubules, while receiving sustenance from another type of cell, the Sertoli cell. The budding *** cells go through a type of division called meiosis—in which each divides twice, producing four new cells. After meiosis, each new cell contains 23 chromosomes, half the usual number, allowing it to combine with the 23 chromosomes found in the female's egg cell.

Before fertilization can happen, the sperm cells undergo a metamorphosis (spermiogenesis) in which they develop flattened, paddle-shaped heads connected to long tails. At this point, the sperm cells move to the epididymis, the coiled tube that connects a testis with the vas deferens. There maturation continues—sperm become motile, for instance. The young sperm cells remain in the epididymis until they are expelled from the body to become potential fertilizers of an egg.

A drug might interfere with almost any stage of this process. It could prevent the stem cells from differentiating into sperm cells, or it might also work on the numerous enzymes and other proteins that regulate the function of Sertoli cells, meiosis and spermiogenesis.

In surveying the various stages for intervention, researchers have suggested that disrupting maturation in the epididymis—where the sperm become mobile and achieve the ability to fertilize an egg—might be the most feasible option. Why? Whether delivered by mouth, by injection or by implant, drugs aimed at altering sperm maturation would have to reach the testes or epididymis via the bloodstream; however, blood-borne drugs often cannot pass out of the circulation and into the part of the testes where sperm are manufactured. Further, many drugs that are capable of stalling sperm synthesis have proved toxic to spermatogonia in the testes and would thus lead to irreversible sterility.

The epididymis presents a number of targets for new drug research. Intervention at the level of the epididymis can both affect sperm count and hamper the ability of sperm to fertilize an egg. One set of investigators has found that triptolide, an isolate from a Chinese plant originally used for treatment of skin diseases and rheumatoid arthritis, affects fertility by hindering sperm motility in the epididymis.

Because triptolide disrupted sperm production, researchers worried that it might cause permanent infertility. More recent studies in rats by Amiya Sinha-Hikim and his colleagues at Harbor University of California at Los Angeles Medical Center have shown that at lower doses, triptolide appears to leave sperm production in the testes intact but reduces the number of active sperm in the epididymis by 70 percent.

During sperm maturation in the epididymis, changes in the sperm's outer lipid plasma membrane take place that allow a biochemical reaction that gives sperm the capability of fertilizing an egg. When it encounters an egg cell, a mature sperm's outer membrane merges with a bag of enzymes at its tip (the acrosome). The enzymes then eat through the egg's outer layer to permit fertilization.

Investigators have explored the potential of the antihypertensive drug nifedipine to inhibit fertility, perhaps by preventing the incorporation of a cell receptor into the plasma membrane while a sperm is in the epididymis. This receptor is needed for the plasma membrane-acrosome reaction to allow the sperm and egg to fuse. Susan Benoff and her colleagues at North Shore University Hospital in Manhasset, N.Y., discovered this contraceptive effect when they found that sperm from some men did not fertilize their mates' eggs during in vitro fertilization. Subsequent sleuthing revealed that the men were taking nifedipine, a calcium channel blocker. Stopping the medication reversed the effect.

Benoff suggests that the drug interferes with the discharge of enzymes from the head of the sperm that are essential for fertilization of the egg. Current studies are attempting to determine whether a calcium channel blocker similar to nifedipine can be designed so that it would affect sperm function but would not decrease blood pressure and heart rate, as nifedipine does.

Study of the epididymis may also suggest other ways to inhibit fertility. During the 10 to 14 days that they develop in the epididymis, sperm acquire cholesterol that prevents them from undergoing prematurely the biochemical reaction between the plasma membrane and the acrosome. Chemicals that disrupt the uptake of cholesterol by sperm in the epididymis—either by starving or by overloading them with the substance—might yield contraceptives that would either block the plasma membrane-acrosome reaction or cause it to take place in the epididymis before it can occur between the sperm and egg. Another strategy for a new contraceptive would hinder the action of antioxidants in the epididymis that protect the plasma membrane from free radical chemicals that could damage it.



hope some of this info could help..

[ghosthunter]

:shocked: back door???:ouch: You don't need any contraceptives for that part.:jawdrop:

ahem... "bareback" action dapat yun.

[ghosthunter]

I used to have lotsa them....

Where's your source now, bro.?.....

8707:soccer:

Watson's has them...

[jonski]

Watson's has them...

Wala ako makita.

[ghosthunter]

Wala ako makita.

Let me check later...

[woohoo]

Rhythm Method coupled with Coitus Interruptus. Pun intended.

[CVT]

Let me check later...

Whew! Kahit sa Norte pa iyan,- dadayuhin ko sigurado.... :hysterical:

8707:soccer:

[mikhael]

:shocked: back door???:ouch: You don't need any contraceptives for that part.:jawdrop:

[SIZE=3]Oh yes, you do! Where do you think politicians come from? [/SIZE]