A Thorough Investigation of the Characteristic Phosphorus Couplings and 31P NMR Analysis in Attempts to Synthesize an Ifosfamide Analog Open Access

Wein, Emily P. (2011)

Permanent URL: https://etd.library.emory.edu/concern/etds/ms35t906v?locale=pt-BR%2A

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Abstract

Cancer remains one of the most prominent global health concerns in today's society.
According to the International Journal of Cancer, there were an estimated 12.7 million
newly reported cancer cases and 7.6 million cancer deaths in 2008.¹ The Cancer Journal for
Clinicians indicated that, in the United States, one in four deaths is caused by cancer.² A
common treatment for cancer is the use of nitrogen mustard chemotherapy treatments that
function by alkylating two different positions of a DNA strand, causing intrastrand
crosslinks (ISCs) or kinks in the DNA structure, as well as severing the base pairs from the
DNA backbone. These chemotherapy treatments, however, have severe side effects due to
their lack of selectivity in the body and their inability to differentiate between cancerous
and healthy dividing cells. This investigation focused on a specific nitrogen mustard
chemotherapy drug, ifosfamide, in efforts to synthesize an analog
of ifosfamide with the added functionality of a double bond in its ring structure.

Once functionality is established in the ring, it opens the possibility of attaching other
ligands to the double bond site on the ring, ligands that could selectively bind the drug to
desired regions in the body.

1 Ferlay, Jacques, et. al. "Estimates of Worldwide Burden of Cancer in 2008: GLOBOCAN 2008." International
Journal of Cancer. 15 December 2010, 127 (12), 2893.
2 Jemal, Ahmedin, et. al. "Cancer Statistics, 2008." Cancer Journal for Clinicians. 2008, 58, 71.

Table of Contents

1. Introduction………………………………………………………………………………….......1
2. Results and Discussion……………………………………….. ………………………...10
2.1 Ifosfamide Characterization…………………………………..……………….…....10
2.2 Addition of Two Equivalents of Chloroethylamine………………….…....17
2.3 Addition of Propargyl Alcohol………………………………..………………,......18
2.4 Flash Chromatography and TLC Difficulties……………………..……….....20
2.5 31P NMR Data and Exploring Impurities……………………………..………..23
2.6 Cyclization Attempts…………………………………………..……………………......30
3. Conclusion and Future Research…………………………………..………………...42
4. Experimental Section…………………………………………..…………………………..45
4.1 General Procedures…….……………………………….. . …………………………...45
4.2 Synthesis of N,N'-Bis(2-chloro-2-ethyl)phosphoramidic chloride.46
4.3 Synthesis of N,N'-Bis(2--chloro-2--ethyl)phosphoramidicpropargylic
ester……………………………………………………………………………………………….......46
4.4 Spectral Data for Ifosfamide………………………………………………………...47
4.5 Initial Attempt at Cyclization………………………………………………….. ....47
4.6 Secondary Attempt at Cyclization………………………………………………...47
4.7 Final Attempt at Cyclization……………………………………………..……….. .48
5. References…………………………………………………………………………….…….....49

About this Honors Thesis

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School	Emory College
Department	Chemistry
Degree	BA
Submission	Honors Thesis
Language	English
Research Field	Chemistry, Organic
Keyword	Synthesis Chemotherapy Ifosfamide
Committee Chair / Thesis Advisor	McDonald, Frank, Emory University
Committee Members	Weinschenk, Matthew, Emory University Sunderam, Vaidy S, Emory University

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