Hormones are chemical messengers that transport signals from one cell to another, the concentration of hormones can be used to determine whether the reproductive system is functioning normally. When hormones are out of balance, a direct effect on the physiological state of the system occurs, and may also increase the risk of cancer. This thesis is organized into two components: the first involves the development of an analytical method utilizing two dimensional ultrahigh-pressure liquid chromatography－tandem mass spectrometry(2D-UHPLC-MS/MS) to investigate the concentration of steroid hormones in the blood, while the second involves the application of the developed method to examine the relations between hormone concentrations to breast cancer risk in premenopausal women. The first component of this research achieved the development of an accurate and sensitive UHPLC-MS/MS method for the determination of the concentrations of estrone, estradiol, estriol, androstendione, testerone, and progesterone in human plasma. As the plasma concentration of estrone, estradiol and estriol tend to be low (around pg mL-1 range), the sensitivity of the method was developed to encompass this range. The developed method utilized a 2D-UHPLC-MS/MS setup, which allows for large injection volumes in order to achieve desirable sensitivity levels. The development of the method included investigation to find the most suitable column, mobile phase composition, pH of buffer solution, ionization source, and MS parameters. Experimental results showed that at higher pH values were able to significantly improve the sensitivity for the detection of estrogens, thus the mobile phase was chosen to be isopropanol and 0.1% triethylamine. The alkali resistant column Gemini C18 was chosen as a result. Androgens and progesterone were analyzed on a Kinetex C18 column, using acetonitrile and 0.1% formic acid as the mobile phase. After the optimization of the chromatographic and MS conditions, the resulting analytical method was able to achieve quantitative limits of 50 pg mL-1, 0.72 pg mL-1, 0.63 pg mL-1, 25 pg mL-1, 12.5 pg mL-1 and50 pg mL-1, respectively for the hormones E3, E2, E1, A, T, and P, with accuracy ranging from 83.80 ± 4.07 to 105.07 ± 4.84%. The linear range covers the concentration ranges of each respective hormone found in premenopausal women. The developed method proved to be a sensitive and accurate analytical method for the detection of 6 hormones in human plasma, and is an accurate and efficient tool that can be applied to hormone related cancer research and evaluation of treatment response. The second component of the study discusses the relative risks and relations between the concentration of hormones (including estrogens and androgens) in premenopausal women and breast cancer. In recent years, the age of breast cancer patients in Taiwan have lowered, statistical data show that the average age of breast cancer patients in Taiwan are much lower than those in western countries. The mechanism of breast cancer occurrence in premenopausal women has not been fully understood. As of now, research relating hormone concentrations to breast cancer are few, and published results from teams within and out of the country are not in agreement. This study utilizes the method developed in part one to measure hormone concentration in both breast cancer patients and healthy controls. Experimental results showed that the estrogen (E1, E2) and androgens showed statistically significant difference (p<0.05) of concentrations between healthy controls and breast cancer patients, while estrogens E3 do not display such a pattern. Within the statistically significant hormones, estrogen E1 was found to have an inverse association with breast cancer risk. However, androgens were found to be positively correlated to breast cancer risk. Although the results were not statistically significant, the estrogens E3 were found to be generally lower in breast cancer patients than in normal controls. These primary experimental results show that hormone concentrations is associated with breast cancer risk in premenopausal women. Although further research with larger patient population are required to validate this assumption. Possible confounding factors, cancer subtypes , and drug treatment responses should also be considered in future work.